Symlin Diabetic Treatment - Symlin Patient Information

Brand Name: Symlin, SymlinPen
Generic Name: pramlintide

Pronounced: PRAM-lin-tide

Symlin, Symlyn Pen, pramlintide, full prescribing information

(Subcutaneous route)

Available Dosage Forms:

  • Solution

Therapeutic Class: Antidiabetic

Subcutaneous route Solution

Pramlintide acetate is used with insulin and has been associated with an increased risk of insulin-induced severe hypoglycemia, particularly in patients with type 1 diabetes. When severe hypoglycemia associated with pramlintide acetate use occurs, it is seen within 3 hours following a pramlintide acetate injection. If severe hypoglycemia occurs while operating a motor vehicle, heavy machinery, or while engaging in other high-risk activities, serious injuries may occur. Appropriate patient selection, careful patient instruction, and insulin dose adjustments are critical elements for reducing this risk .

Pramlintide acetate is used with insulin and has been associated with an increased risk of insulin-induced severe hypoglycemia. When severe hypoglycemia associated with pramlintide acetate use occurs, it is seen within 3 hours following a pramlintide acetate injection. Appropriate patient selection, careful patient instruction, and insulin dose adjustments are critical elements for reducing this risk .

Uses For Symlin

Pramlintide is used to control blood sugar in patients with type 1 and type 2 diabetes. It is always used with insulin.

This medicine is available only with your doctor's prescription.

Before Using Symlin

In deciding to use a medicine, the risks of taking the medicine must be weighed against the good it will do. This is a decision you and your doctor will make. For this medicine, the following should be considered:


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Allergies

Tell your doctor if you have ever had any unusual or allergic reaction to this medicine or any other medicines. Also tell your health care professional if you have any other types of allergies, such as to foods, dyes, preservatives, or animals. For non-prescription products, read the label or package ingredients carefully.

Pediatric

Studies on this medicine have been done only in adult patients, and there is no specific information comparing use of pramlintide in children with use in other age groups.

Geriatric

This medicine has been tested and has not been shown to cause different side effects or problems in older people than it does in younger adults. However, some elderly people may be especially sensitive to the effects of low blood sugar. The doctor should manage pramlintide and insulin treatment to prevent an increased risk of severely low blood sugar.

Pregnancy

 Pregnancy CategoryExplanation
All Trimesters C Animal studies have shown an adverse effect and there are no adequate studies in pregnant women OR no animal studies have been conducted and there are no adequate studies in pregnant women.

Breast Feeding

There are no adequate studies in women for determining infant risk when using this medication during breastfeeding. Weigh the potential benefits against the potential risks before taking this medication while breastfeeding.

Interactions with Medicines

Although certain medicines should not be used together at all, in other cases two different medicines may be used together even if an interaction might occur. In these cases, your doctor may want to change the dose, or other precautions may be necessary. Tell your healthcare professional if you are taking any other prescription or nonprescription (over-the-counter [OTC]) medicine.

Interactions with Food/Tobacco/Alcohol

Certain medicines should not be used at or around the time of eating food or eating certain types of food since interactions may occur. Using alcohol or tobacco with certain medicines may also cause interactions to occur. Discuss with your healthcare professional the use of your medicine with food, alcohol, or tobacco.

Other Medical Problems

The presence of other medical problems may affect the use of this medicine. Make sure you tell your doctor if you have any other medical problems, especially:

  • Gastroparesis (a condition where the stomach takes too long to empty its contents) or
  • HbA1c9% (lab test that shows too high or low amount of sugar in the blood) or
  • Hypoglycemia unawareness (unable to recognize symptoms of low blood sugar until it becomes severe) or
  • Severe hypoglycemia (severe low blood sugar that comes back and has required assistance from medical personnel in the past 6 months)—If you have any of these conditions, you should NOT take pramlintide.
  • Hypoglycemia, insulin-induced, history of (low blood sugar brought on by using insulin in the past)—May increase risk of severe hypoglycemia occurring again

Proper Use of Pramlintide

This section provides information on the proper use of a number of products that contain pramlintide. It may not be specific to Symlin. Please read with care.

Dosing

The dose of this medicine will be different for different patients. Follow your doctor's orders or the directions on the label. The following information includes only the average doses of this medicine. If your dose is different, do not change it unless your doctor tells you to do so.

The amount of medicine that you take depends on the strength of the medicine. Also, the number of doses you take each day, the time allowed between doses, and the length of time you take the medicine depend on the medical problem for which you are using the medicine.

It is important to follow any instructions from your doctor about the careful selection and rotation of injection sites on your body.

You should never mix your insulin and pramlintide injections. These injections should be done separately. If you have questions about this, ask your doctor or pharmacist.

  • For injection dosage form:
    • Diabetes, type 1 or type 2
      • Adults—The dose is based on your blood sugar and how well your body adjusts to the medicine. This must be determined by your doctor. The medicine is injected under the skin in your abdomen or thigh right before major meals. Also, your doctor will reduce your insulin dose by half before you begin receiving pramlintide.
      • Children—Use and dose must be determined by your doctor.

Missed Dose

Call your doctor or pharmacist for instructions.

Storage

Store in the refrigerator. Do not freeze.

A pramlintide vial in use may be kept in the refrigerator or at room temperature for up to 28 days. An open vial of pramlintide that has been kept in the refrigerator or at room temperature for longer than 28 days should be thrown away. Storing prefilled syringes in the refrigerator with the needle pointed up reduces problems that can occur, such as crystals forming in the needle and blocking it up.

Precautions While Using Symlin

It is very important that your doctor check your progress at regular visits, especially during the first few weeks of pramlintide treatment.

It is very important to follow carefully any instructions from your health care team about:

  • Alcohol—Drinking alcohol may cause severe low blood sugar. Discuss this with your health care team.
  • Other medicines—Do not take other medicines unless they have been discussed with your doctor. This especially includes nonprescription medicines such as aspirin, and medicines for appetite control, asthma, colds, cough, hay fever, or sinus problems.
  • Counseling—Other family members need to learn how to prevent side effects or help with side effects if they occur. Also, patients with diabetes, especially teenagers, may need special counseling about pramlintide dosing changes that might occur because of lifestyle changes, such as changes in exercise and diet. Furthermore, counseling on contraception and pregnancy may be needed because of the problems that can occur in women with diabetes who become pregnant.
  • Travel—Keep a recent prescription and your medical history with you. Be prepared for an emergency as you would normally. Make allowances for changing time zones, keep your meal times as close as possible to your usual meal times, and store pramlintide properly.

In case of emergency—There may be a time when you need emergency help for a problem caused by your diabetes. You need to be prepared for these emergencies. It is a good idea to:

  • Wear a medical identification (ID) bracelet or neck chain at all times. Also, carry an ID card in your wallet or purse that says that you have diabetes and lists all of your medicines.
  • Keep an extra supply of insulin and syringes with needles on hand in case high blood sugar occurs.
  • Keep some kind of quick-acting sugar handy to treat low blood sugar.
  • Have a glucagon kit available in case severe low blood sugar occurs. Check and replace any expired kits regularly.

Too much insulin can cause low blood sugar (also called hypoglycemia or insulin reaction). Symptoms of low blood sugar must be treated before they lead to unconsciousness (passing out). Different people may feel different symptoms of low blood sugar. It is important that you learn what symptoms of low blood sugar you usually have so that you can treat it quickly.

  • Symptoms of low blood sugar can include: anxious feeling, behavior change similar to being drunk, blurred vision, cold sweats, confusion, cool pale skin, difficulty in concentrating, drowsiness, excessive hunger, fast heartbeat, headache, nausea, nervousness, nightmares, restless sleep, shakiness, slurred speech, and unusual tiredness or weakness.
  • The symptoms of low blood sugar may develop quickly and may result from:
    • delaying or missing a scheduled meal or snack.
    • exercising more than usual.
    • drinking a significant amount of alcohol.
    • taking certain medicines.
    • using too much insulin.
    • sickness (especially with vomiting or diarrhea).
  • Know what to do if symptoms of low blood sugar occur. Eating some form of quick-acting sugar when symptoms of low blood sugar first appear will usually prevent them from getting worse. Good sources of sugar include:
    • Glucose tablets or gel, fruit juice or nondiet soft drink (4 to 6 ounces [one-half cup]), corn syrup or honey (1 tablespoon), sugar cubes (six one-half inch size), or table sugar (dissolved in water).
      • If a snack is not scheduled for an hour or more you should also eat a light snack, such as cheese and crackers, half a sandwich, or drink an 8-ounce glass of milk.
      • Do not use chocolate because its fat slows down the sugar entering into the blood stream.
    • Glucagon is used in emergency situations such as unconsciousness. Have a glucagon kit available and know how to prepare and use it. Members of your household also should know how and when to use it.

High blood sugar (hyperglycemia) is another problem related to uncontrolled diabetes. If you have any symptoms of high blood sugar, contact your health care team right away. If high blood sugar is not treated, severe hyperglycemia can occur, leading to ketoacidosis (diabetic coma) and death.

  • The symptoms of mild high blood sugar appear more slowly than those of low blood sugar. Symptoms can include: blurred vision; drowsiness; dry mouth; flushed and dry skin; fruit-like breath odor; increased urination (frequency and volume); loss of appetite; stomachache, nausea, or vomiting; tiredness; troubled breathing (rapid and deep); and unusual thirst.
  • Symptoms of severe high blood sugar (called ketoacidosis or diabetic coma) that need immediate hospitalization include: flushed and dry skin, fruit-like breath odor, ketones in urine, passing out, and troubled breathing (rapid and deep).
  • High blood sugar symptoms may occur if you:
    • have diarrhea, a fever, or an infection.
    • do not take enough insulin or skip a dose of insulin.
    • do not exercise as much as usual.
    • overeat or do not follow your meal plan.
  • Know what to do if high blood sugar occurs. Your doctor may recommend changes in your pramlintide and/or insulin dose or meal plan to avoid high blood sugar. Symptoms of high blood sugar must be corrected before they progress to more serious conditions. Check with your doctor often to make sure you are controlling your blood sugar. Your doctor might discuss the following with you:
    • Increasing your insulin dose when you plan to eat an unusually large dinner, such as on holidays. This type of increase is called an anticipatory dose.
    • Decreasing your dose for a short time for special needs, such as when you cannot exercise as you normally do. Changing only one type of insulin dose (usually the first dose) and anticipating how the change may affect other doses during the day. Contacting your doctor if you need a permanent change in dose.
    • Delaying a meal if your blood glucose is over 200 mg/dL to allow time for your blood sugar to go down. An extra insulin dose may be needed if your blood sugar does not come down shortly.
    • Not exercising if your blood glucose is over 240 mg/dL and reporting this to your doctor immediately.
    • Being hospitalized if ketoacidosis or diabetic coma occurs.

Symlin Side Effects

Along with its needed effects, a medicine may cause some unwanted effects. Although not all of these side effects may occur, if they do occur they may need medical attention.

Check with your doctor immediately if any of the following side effects occur:

More common

  • Anxiety
  • blurred vision
  • chills
  • cold sweats
  • coma
  • confusion
  • cool pale skin
  • cough
  • depression
  • difficulty swallowing
  • dizziness
  • fast heartbeat
  • headache
  • hives
  • increased hunger
  • itching
  • nausea
  • nervousness
  • nightmares
  • puffiness or swelling of the eyelids or around the eyes, face, lips, or tongue
  • seizures
  • shakiness
  • shortness of breath
  • skin rash
  • slurred speech
  • tightness in chest
  • unusual tiredness or weakness
  • wheezing

Some side effects may occur that usually do not need medical attention. These side effects may go away during treatment as your body adjusts to the medicine. Also, your health care professional may be able to tell you about ways to prevent or reduce some of these side effects. Check with your health care professional if any of the following side effects continue or are bothersome or if you have any questions about them:

More common

  • Difficulty in moving
  • inflicted injury
  • loss of appetite
  • muscle pain or stiffness
  • pain in joints
  • stomach pain
  • vomiting
  • weight loss

Less common

  • Body aches or pain
  • congestion
  • dryness or soreness of throat
  • fever
  • hoarseness
  • runny nose
  • tender, swollen glands in neck
  • trouble in swallowing
  • voice changes

Other side effects not listed may also occur in some patients. If you notice any other effects, check with your healthcare professional.

Last Updated: 07/2008

Symlin, Symlyn Pen, pramlintide, full prescribing information

Detailed Info on Signs, Symptoms, Causes, Treatments of Diabetes

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APA Reference
Staff, H. (2008, July 31). Symlin Diabetic Treatment - Symlin Patient Information, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/diabetes/medications/symlin-type-2-diabetes-treatment

Last Updated: July 18, 2014

Symlin for Treatment of Diabetes - Symlin Full Prescribing Information

Brand Name: Symlin, Symlin Pen
Generic Name: pramlintide acetate

Contents:

Description
Pharmacology
Clinical Studies
Indications and Usage
Contraindications
Warnings
Precautions
Adverse Reactions
Overdose
Dosage and Administration
How Supplied
Storage

Symlin, Symlin Pen, pramlintide acetate, patient information (in plain English)

WARNING

Symlin is used with insulin and has been associated with an increased risk of insulin-induced severe hypoglycemia, particularly in patients with type 1 diabetes. When severe hypoglycemia associated with Symlin use occurs, it is seen within 3 hours following a Symlin injection. If severe hypoglycemia occurs while operating a motor vehicle, heavy machinery, or while engaging in other high-risk activities, serious injuries may occur. Appropriate patient selection, careful patient instruction, and insulin dose adjustments are critical elements for reducing this risk.

Description

Symlin® (pramlintide acetate) injection is an antihyperglycemic drug for use in patients with diabetes treated with insulin. Pramlintide is a synthetic analog of human amylin, a naturally occurring neuroendocrine hormone synthesized by pancreatic beta cells that contributes to glucose control during the postprandial period. Pramlintide is provided as an acetate salt of the synthetic 37-amino acid polypeptide, which differs in amino acid sequence from human amylin by replacement with proline at positions 25 (alanine), 28 (serine), and 29 (serine).

The structural formula of pramlintide acetate is as shown:

Structural formula of pramlintide acetate

Pramlintide acetate is a white powder that has a molecular formula of C171H267N51O53S2- x C2H4O2 (3≤x≤8); the molecular weight is 3949.4. Pramlintide acetate is soluble in water.

Symlin is formulated as a clear, isotonic, sterile solution for subcutaneous (SC) administration. The disposable multidose SymlinPen® pen-injector contains 1000 mcg/mL of pramlintide (as acetate); Symlin vials contain 600 mcg/mL of pramlintide (as acetate). Both formulations contain 2.25 mg/mL of metacresol as a preservative, D-mannitol as a tonicity modifier, and acetic acid and sodium acetate as pH modifiers. Symlin has a pH of approximately 4.0.


 


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Clinical Pharmacology

Amylin Physiology

Amylin is co-located with insulin in secretory granules and co-secreted with insulin by pancreatic beta cells in response to food intake. Amylin and insulin show similar fasting and postprandial patterns in healthy individuals (Figure 1).

Secretion Profile of Amylin and Insulin in Healthy Adults

Figure 1: Secretion Profile of Amylin and Insulin in Healthy Adults

Amylin affects the rate of postprandial glucose appearance through a variety of mechanisms. Amylin slows gastric emptying (i.e., the rate at which food is released from the stomach to the small intestine) without altering the overall absorption of nutrients. In addition, amylin suppresses glucagon secretion (not normalized by insulin alone), which leads to suppression of endogenous glucose output from the liver. Amylin also regulates food intake due to centrally-mediated modulation of appetite.

In patients with insulin-using type 2 or type 1 diabetes, the pancreatic beta cells are dysfunctional or damaged, resulting in reduced secretion of both insulin and amylin in response to food.

Mechanism of Action

Symlin, by acting as an amylinomimetic agent, has the following effects: 1) modulation of gastric emptying; 2) prevention of the postprandial rise in plasma glucagon; and 3) satiety leading to decreased caloric intake and potential weight loss.

Gastric Emptying

The gastric-emptying rate is an important determinant of the postprandial rise in plasma glucose. Symlin slows the rate at which food is released from the stomach to the small intestine following a meal and, thus, it reduces the initial postprandial increase in plasma glucose. This effect lasts for approximately 3 hours following Symlin administration. Symlin does not alter the net absorption of ingested carbohydrate or other nutrients.

Postprandial Glucagon Secretion

In patients with diabetes, glucagon concentrations are abnormally elevated during the postprandial period, contributing to hyperglycemia. Symlin has been shown to decrease postprandial glucagon concentrations in insulin-using patients with diabetes.
Satiety

Symlin administered prior to a meal has been shown to reduce total caloric intake. This effect appears to be independent of the nausea that can accompany Symlin treatment.

Pharmacokinetics

Absorption

The absolute bioavailability of a single SC dose of Symlin is approximately 30 to 40%. Subcutaneous administration of different doses of Symlin into the abdominal area or thigh of healthy subjects resulted in dose-proportionate maximum plasma concentrations (Cmax) and overall exposure (expressed as area under the plasma concentration curve or (AUC)) (Table 1).

Table 1: Mean Pharmacokinetic Parameters Following Administration of Single SC Doses of Symlin

SC Dose
(mcg)
AUC (0-β)
(pmol*min/L)
Cmax
(pmol/L)
Tmax
(min)
Elimination t ½
(min)
30 3750 39 21 55
60 6778 79 20 49
90 8507 102 19 51
120 11970 147 21 48

Injection of Symlin into the arm showed higher exposure with greater variability, compared with exposure after injection of Symlin into the abdominal area or thigh.

There was no strong correlation between the degree of adiposity as assessed by BMI or skin fold thickness measurements and relative bioavailability. Injections administered with 6.0-mm and 12.7-mm needles yielded similar bioavailability.

Distribution

Symlin does not extensively bind to blood cells or albumin (approximately 40% of the drug is unbound in plasma), and thus Symlin's pharmacokinetics should be insensitive to changes in binding sites.

Metabolism and Elimination

In healthy subjects, the half-life of Symlin is approximately 48 minutes. Symlin is metabolized primarily by the kidneys. Des-lys1 pramlintide (2-37 pramlintide), the primary metabolite, has a similar half-life and is biologically active both in vitro and in vivo in rats. AUC values are relatively constant with repeat dosing, indicating no bioaccumulation.

Special Populations

Renal Insufficiency

Patients with moderate or severe renal impairment (ClCr>20 to ≤50 mL/min) did not show increased Symlin exposure or reduced Symlin clearance, compared to subjects with normal renal function. No studies have been done in dialysis patients.

Hepatic Insufficiency

Pharmacokinetic studies have not been conducted in patients with hepatic insufficiency. However, based on the large degree of renal metabolism (see Metabolism and Elimination), hepatic dysfunction is not expected to affect blood concentrations of Symlin.

Geriatric

Pharmacokinetic studies have not been conducted in the geriatric population. Symlin should only be used in patients known to fully understand and adhere to proper insulin adjustments and glucose monitoring. No consistent age-related differences in the activity of Symlin have been observed in the geriatric population (n=539 for patients 65 years of age or older in the clinical trials).

Pediatric

Symlin has not been evaluated in the pediatric population.

Gender

No study has been conducted to evaluate possible gender effects on Symlin pharmacokinetics. However, no consistent gender-related differences in the activity of Symlin have been observed in the clinical trials (n=2799 for male and n=2085 for female).

Race/Ethnicity

No study has been conducted to evaluate the effect of ethnicity on Symlin pharmacokinetics. However, no consistent differences in the activity of Symlin have been observed among patients of differing race/ethnicity in the clinical trials (n=4257 for white, n=229 for black, n=337 for Hispanic, and n=61 for other ethnic origins).

Drug Interactions

The effect of Symlin (120 mcg) on acetaminophen (1000 mg) pharmacokinetics as a marker of gastric-emptying was evaluated in patients with type 2 diabetes (n=24). Symlin did not significantly alter the AUC of acetaminophen. However, Symlin decreased acetaminophen Cmax (about 29% with simultaneous co-administration) and increased the time to maximum plasma concentration or tmax (ranging from 48 to 72 minutes) dependent on the time of acetaminophen administration relative to Symlin injection. Symlin did not significantly affect acetaminophen tmax when acetaminophen was administered 1 to 2 hours before Symlin injection. However, the tmax of acetaminophen was significantly increased when acetaminophen was administered simultaneously with or up to 2 hours following Symlin injection (see PRECAUTIONS, Drug Interactions).

Pharmacodynamics

In clinical studies in patients with insulin-using type 2 and type 1 diabetes, Symlin administration resulted in a reduction in mean postprandial glucose concentrations, reduced glucose fluctuations, and reduced food intake. Symlin doses differ for insulin-using type 2 and type 1 patients (see DOSAGE AND ADMINISTRATION).

Reduction in Postprandial Glucose Concentrations

Symlin administered subcutaneously immediately prior to a meal reduced plasma glucose concentrations following the meal when used with regular insulin or rapid-acting insulin analogs (Figure 2). This reduction in postprandial glucose decreased the amount of short-acting insulin required and limited glucose fluctuations based upon 24-hour glucose monitoring. When rapid-acting analog insulins were used, plasma glucose concentrations tended to rise during the interval between 150 minutes following Symlin injection and the next meal (see DOSAGE AND ADMINISTRATION).

Postprandial Plasma Glucose Profiles in Patients With Type 2 and Type 1 Diabetes Receiving Symlin and/or Insulin

Figure 2: Postprandial Plasma Glucose Profiles in Patients With Type 2 and Type 1 Diabetes Receiving Symlin and/or Insulin

Reduced Food Intake

A single, subcutaneous dose of Symlin 120 mcg (type 2) or 30 mcg (type 1) administered 1 hour prior to an unlimited buffet meal was associated with reductions in total caloric intake (placebo-subtracted mean changes of ~23% and 21%, respectively), which occurred without decreases in meal duration.

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Clinical Studies

A total of 5325 patients and healthy volunteers received Symlin in clinical studies. This includes 1688 with type 2 diabetes and 2375 with type 1 diabetes in short- and long-term controlled clinical trials, long-term uncontrolled clinical trials, and an open-label study in the clinical practice setting.

Clinical Studies in Type 2 Diabetes

The efficacy of a range of Symlin doses was evaluated in several placebo-controlled and open-label clinical trials in insulin-using patients with type 2 diabetes. Based on results obtained in these studies, the recommended dose of Symlin for patients with insulin-using type 2 diabetes is 120 mcg administered immediately prior to major meals.

Two, long-term (26 to 52 week), randomized, double-blind, placebo-controlled studies of Symlin were conducted in patients with type 2 diabetes using fixed dose insulin to isolate the Symlin effect. Demographic and baseline characteristics for the 871 Symlin-treated patients are as follows: mean baseline HbA1c ranged from 9.0 to 9.4%, mean age was 56.4 to 59.1 years, mean duration of diabetes ranged from 11.5 to 14.4 years, and mean BMI ranged from 30.1 to 34.4 kg/m2. In both of these studies, Symlin or placebo was added to the participants' existing diabetes therapies, which included insulin with or without a sulfonylurea agent and/or metformin.

Table 2 summarizes the composite results across both studies for patients assigned to the 120-mcg dose after 6 months of treatment.

Table 2: Mean (SE) Change in HbA1c, Weight, and Insulin at 6 Months in the Double-Blind, Placebo-Controlled Studies in Patients With Insulin-Using Type 2 Diabetes

VariablePlaceboSymlin (120 mcg)
Baseline HbA1c (%) 9.3 (0.08) 9.1 (0.06)
Change in HbA1c at 6 Months Relative to Baseline (%) −0.17 (0.07) −0.57 (0.06)*
Placebo-Subtracted HbA1c Change at 6 Months (%) NA −0.40 (0.09)*
Baseline Weight (kg) 91.3 (1.2) 92.5 (1.2)
Change in Weight at 6 Months Relative to Baseline (kg) +0.2 (0.2) −1.5 (0.2)*
Placebo-Subtracted Weight Change at 6 Months (kg) NA −1.7 (0.3)*
Percent Change in Insulin Doses at 6 Months: Rapid/Short-Acting +6.5 (2.7) −3.0 (1.6)*
Percent Change in Insulin Doses at 6 Months: Long-Acting +5.2 (1.4) −0.2 (1.3)*

* Statistically significant reduction compared with placebo (p-value < 0.05).

In a cohort of 145 patients who completed two years of Symlin treatment the baseline-subtracted HbA1c and weight reductions were: −0.40% and −0.36 kg, respectively.

Open-Label Study in the Clinical Practice Setting

An open-label study of Symlin was conducted at the recommended dose of 120 mcg in 166 patients with insulin-using type 2 diabetes who were unable to achieve glycemic targets using insulin alone. A flexible-dose insulin regimen was employed in these patients (see DOSAGE AND ADMINISTRATION). In this study, patients adjusted their insulin regimen based on pre- and post-meal glucose monitoring. At baseline, mean HbA1c was 8.3%, mean age was 54.4 years, mean duration of diabetes was 13.3 years, and mean BMI was 38.6 kg/m2. Symlin was administered with major meals. Symlin plus insulin treatment for 6 months resulted in a baseline-subtracted mean HbA1c reduction of −0.56 ± 0.15% and a baseline-subtracted mean weight reduction of −2.76 ± 0.34 kg. These changes were accomplished with reductions in doses of total, short-acting, and long-acting insulin (−6.4 ± 2.66, −10.3 ± 4.84, and −4.20 ± 2.42%, respectively).

Clinical Studies in Type 1 Diabetes

The efficacy of a range of Symlin doses was evaluated in several placebo-controlled and open-label clinical trials conducted in patients with type 1 diabetes. Based on results obtained in these studies, the recommended dose of Symlin for patients with type 1 diabetes is 30 mcg or 60 mcg administered immediately prior to major meals.

Three, long-term (26 to 52 week), randomized, double-blind, placebo-controlled studies of Symlin were conducted in patients with type 1 diabetes (N=1717). Two of these studies allowed only minimal insulin adjustments in order to isolate the Symlin effect; in the third study, insulin adjustments were made according to standard medical practice. Demographic and baseline characteristics for the 1179 Symlin-treated patients were as follows: mean baseline HbA1c range was 8.7 to 9.0%, mean age range was 37.3 to 41.9 years, mean duration of diabetes range was 15.5 to 19.2 years, and mean BMI range was 25.0 to 26.8 kg/m2. Symlin or placebo was added to existing insulin therapies.

Table 3 summarizes the composite results across these studies for patients assigned to the 30 or 60 mcg dose after 6 months of treatment.

Table 3: Mean (SE) Change in HbA1c, Weight, and Insulin at 6 Months in the Double-Blind, Placebo-Controlled Studies in Patients With Type 1 Diabetes

VariablePlaceboSymlin
(30 or 60 mcg)
Baseline HbA1c (%) 9.0 (0.06) 8.9 (0.04)
Change in HbA1c at 6 Months Relative to Baseline (%) −0.10 (0.05) −0.43 (0.04)*
Placebo-Subtracted HbA1c Change at 6 Months (%) NA −0.33 (0.06)*
Baseline Weight (kg) 75.1 (0.6) 76.1 (0.5)
Change in Weight at 6 Months Relative to Baseline (kg) +0.6 (0.1) −1.1 (0.1)*
Placebo-Subtracted Weight Change at 6 Months (kg) NA −1.7 (0.1)*
Percent Change in Insulin Doses at 6 Months: Rapid/Short-Acting +1.7 (3.3) −3.6 (2.9)
Percent Change in Insulin Doses at 6 Months: Long-Acting +2.5 (1.9) +1.9 (1.3)

* Statistically significant reduction compared with placebo (p-value < 0.05).

In a cohort of 73 patients who completed two years of Symlin treatment the baseline-subtracted HbA1c and weight changes were: −0.35% and 0.60 kg, respectively.

Symlin Dose-Titration Trial

A dose-titration study of Symlin was conducted in patients with type 1 diabetes. Patients with relatively good baseline glycemic control (mean HbA1c = 8.1%) were randomized to receive either insulin plus placebo or insulin plus Symlin. Other baseline and demographics characteristics were: mean age of 41 years, mean duration of diabetes of 20 years, mean BMI of 28 kg/m2. Symlin was initiated at a dose of 15 mcg and titrated upward at weekly intervals by 15-mcg increments to doses of 30 mcg or 60 mcg, based on whether patients experienced nausea. Once a tolerated dose of either 30 mcg or 60 mcg was reached, the Symlin dose was maintained for the remainder of the study (Symlin was administered before major meals). During Symlin titration, the insulin dose (mostly the short/rapid-acting insulin) was reduced by 30-50% in order to reduce the occurrence of hypoglycemia. Once a tolerated Symlin dose was reached, insulin dose adjustments were made according to standard clinical practice, based on pre- and post-meal blood glucose monitoring. By 6 months of treatment, patients treated with Symlin and insulin and patients treated with insulin and placebo had equivalent reductions in mean HbA1c (−0.47 ± 0.07% vs. −0.49 ± 0.07%, respectively); patients on Symlin lost weight (−1.33 ± 0.31 kg relative to baseline and −2.6 kg relative to placebo plus insulin-treated patients). Symlin-treated patients used less total insulin (−11.7% relative to baseline) and less short/rapid-acting insulin (−22.8%) relative to baseline.

Open-Label Study in the Clinical Practice Setting

An open-label study of Symlin was conducted in patients with type 1 diabetes who were unable to achieve glycemic targets using insulin alone. A flexible-dose insulin regimen was employed in these patients after Symlin titration was completed (see DOSAGE AND ADMINISTRATION). In this study, patients adjusted their insulin regimen based on pre- and post-meal glucose monitoring. At baseline, mean HbA1c was 8.0%, mean age was 42.7 years, mean duration of diabetes was 21.2 years, and mean BMI was 28.6 kg/m2. Symlin daily dosage was 30 mcg or 60 mcg with major meals.

Symlin plus insulin reduced HbA1c and body weight from baseline at 6 months by a mean of 0.18% and 3.0 kg, respectively. These changes in glycemic control and body weight were achieved with reductions in doses of total, short-acting, and long-acting insulin (−12.0 ± 1.36, −21.7 ± 2.81, and −0.4 ± 1.59%, respectively).

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Indications and Usage

Symlin is given at mealtimes and is indicated for:

  • Type 1 diabetes, as an adjunct treatment in patients who use mealtime insulin therapy and who have failed to achieve desired glucose control despite optimal insulin therapy.
  • Type 2 diabetes, as an adjunct treatment in patients who use mealtime insulin therapy and who have failed to achieve desired glucose control despite optimal insulin therapy, with or without a concurrent sulfonylurea agent and/or metformin.

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Contraindications

Symlin is contraindicated in patients with any of the following:

  • a known hypersensitivity to Symlin or any of its components, including metacresol;
  • a confirmed diagnosis of gastroparesis;
  • hypoglycemia unawareness.

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Warnings

Patient Selection
Proper patient selection is critical to safe and effective use of Symlin

Before initiation of therapy, the patient's HbA1c, recent blood glucose monitoring data, history of insulin-induced hypoglycemia, current insulin regimen, and body weight should be reviewed. Symlin therapy should only be considered in patients with insulin-using type 2 or type 1 diabetes who fulfill the following criteria:

  • have failed to achieve adequate glycemic control despite individualized insulin management;
  • are receiving ongoing care under the guidance of a healthcare professional skilled in the use of insulin and supported by the services of diabetes educator(s).

Patients meeting any of the following criteria should NOT be considered for Symlin therapy:

  • poor compliance with current insulin regimen;
  • poor compliance with prescribed self-blood glucose monitoring;
  • have an HbA1c > 9%;
  • recurrent severe hypoglycemia requiring assistance during the past 6 months;
  • presence of hypoglycemia unawareness;
  • confirmed diagnosis of gastroparesis;
  • require the use of drugs that stimulate gastrointestinal motility;
  • pediatric patients.

Hypoglycemia

Symlin alone does not cause hypoglycemia. However, Symlin is indicated to be co-administered with insulin therapy and in this setting Symlin increases the risk of insulin-induced severe hypoglycemia, particularly in patients with type 1 diabetes. Severe hypoglycemia associated with Symlin occurs within the first 3 hours following a Symlin injection. If severe hypoglycemia occurs while operating a motor vehicle, heavy machinery, or while engaging in other high-risk activities, serious injuries may occur. Therefore, when introducing Symlin therapy, appropriate precautions need to be taken to avoid increasing the risk for insulin-induced severe hypoglycemia. These precautions include frequent pre- and post-meal glucose monitoring combined with an initial 50% reduction in pre-meal doses of short-acting insulin (see DOSAGE AND ADMINISTRATION).

Symptoms of hypoglycemia may include hunger, headache, sweating, tremor, irritability, or difficulty concentrating. Rapid reductions in blood glucose concentrations may induce such symptoms regardless of glucose values. More severe symptoms of hypoglycemia include loss of consciousness, coma, or seizure.

Early warning symptoms of hypoglycemia may be different or less pronounced under certain conditions, such as long duration of diabetes; diabetic nerve disease; use of medications such as beta-blockers, clonidine, guanethidine, or reserpine; or intensified diabetes control.

The addition of any antihyperglycemic agent such as Symlin to an existing regimen of one or more antihyperglycemic agents (e.g., insulin, sulfonylurea), or other agents that can increase the risk of hypoglycemia may necessitate further insulin dose adjustments and particularly close monitoring of blood glucose.

The following are examples of substances that may increase the blood glucose-lowering effect and susceptibility to hypoglycemia: oral anti-diabetic products, ACE inhibitors, diisopyramide, fibrates, fluoxetine, MAO inhibitors, pentoxifylline, propoxyphene, salicylates, and sulfonamide antibiotics.

Clinical studies employing a controlled hypoglycemic challenge have demonstrated that Symlin does not alter the counter-regulatory hormonal response to insulin-induced hypoglycemia. Likewise, in Symlin-treated patients, the perception of hypoglycemic symptoms was not altered with plasma glucose concentrations as low as 45 mg/dL.

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Precautions

General

Hypoglycemia (See WARNINGS).

Symlin should be prescribed with caution to persons with visual or dexterity impairment.

Information for Patients

Healthcare providers should inform patients of the potential risks and advantages of Symlin therapy. Healthcare providers should also inform patients about self-management practices including glucose monitoring, proper injection technique, timing of dosing, and proper storage of Symlin. In addition, reinforce the importance of adherence to meal planning, physical activity, recognition and management of hypoglycemia and hyperglycemia, and assessment of diabetes complications. Refer patients to the Symlin Medication Guide and Patient Instructions for Use for additional information.

Instruct patients on handling of special situations such as intercurrent conditions (illness or stress), an inadequate or omitted insulin dose, inadvertent administration of increased insulin or Symlin dose, inadequate food intake or missed meals.

Symlin and insulin should always be administered as separate injections and never be mixed.

Women with diabetes should be advised to inform their healthcare professional if they are pregnant or contemplating pregnancy.


 


Renal Impairment

The dosing requirements for Symlin are not altered in patients with moderate or severe renal impairment (ClCr >20 to ≤50 mL/min). No studies have been done in dialysis patients (see CLINICAL PHARMACOLOGY; Special Populations).

Hepatic Impairment

Studies have not been performed in patients with hepatic impairment. However, hepatic dysfunction is not expected to affect blood concentrations of Symlin (see CLINICAL PHARMACOLOGY; Special Populations).

Allergy

Local Allergy

Patients may experience redness, swelling, or itching at the site of injection. These minor reactions usually resolve in a few days to a few weeks. In some instances, these reactions may be related to factors other than Symlin, such as irritants in a skin cleansing agent or improper injection technique.

Systemic Allergy

In controlled clinical trials up to 12 months, potential systemic allergic reactions were reported in 65 (5%) of type 2 patients and 59 (5%) of type 1 Symlin-treated patients. Similar reactions were reported by 18 (4%) and 28 (5%) of placebo-treated type 2 and type 1 patients, respectively. No patient receiving Symlin was withdrawn from a trial due to a potential systemic allergic reaction.

Drug Interactions

Due to its effects on gastric emptying, Symlin therapy should not be considered for patients taking drugs that alter gastrointestinal motility (e.g., anticholinergic agents such as atropine) and agents that slow the intestinal absorption of nutrients (e.g., α-glucosidase inhibitors). Patients using these drugs have not been studied in clinical trials.

Symlin has the potential to delay the absorption of concomitantly administered oral medications. When the rapid onset of a concomitant orally administered agent is a critical determinant of effectiveness (such as analgesics), the agent should be administered at least 1 hour prior to or 2 hours after Symlin injection.

In clinical trials, the concomitant use of sulfonylureas or biguanides did not alter the adverse event profile of Symlin. No formal interaction studies have been performed to assess the effect of Symlin on the kinetics of oral antidiabetic agents.

Mixing Symlin and Insulin

The pharmacokinetic parameters of Symlin were altered when mixed with regular, NPH, and 70/30 premixed formulations of recombinant human insulin immediately prior to injection. Thus, Symlin and insulin should not be mixed and must be administered separately.

Carcinogenesis, Mutagenesis, Impairment of Fertility

Carcinogenesis

A two-year carcinogenicity study was conducted in CD-1 mice with doses of 0.2, 0.5, and 1.2 mg/kg/day of Symlin (32, 67, and 159 times the exposure resulting from the maximum recommended human dose based on area under the plasma concentration curve or AUC, respectively). No drug-induced tumors were observed. A two-year carcinogenicity study was conducted in Sprague-Dawley rats with doses of 0.04, 0.2, and 0.5 mg/kg/day of Symlin (3, 9, and 25 times the exposure resulting from the maximum recommended human dose based on AUC, respectively). No drug-induced tumors were observed in any organ.

Mutagenesis

Symlin was not mutagenic in the Ames test and did not increase chromosomal aberration in the human lymphocytes assay. Symlin was not clastogenic in the in vivo mouse micronucleus test or in the chromosomal aberration assay utilizing Chinese hamster ovary cells.

Impairment of Fertility

Administration of 0.3, 1, or 3 mg/kg/day of Symlin (8, 17, and 82 times the exposure resulting from the maximum recommended human dose based on body surface area) had no significant effects on fertility in male or female rats. The highest dose of 3 mg/kg/day resulted in dystocia in 8/12 female rats secondary to significant decreases in serum calcium levels.

Pregnancy

Teratogenic Effects: Pregnancy Category C

No adequate and well-controlled studies have been conducted in pregnant women. Studies in perfused human placenta indicate that Symlin has low potential to cross the maternal/fetal placental barrier. Embryofetal toxicity studies with Symlin have been performed in rats and rabbits. Increases in congenital abnormalities (neural tube defect, cleft palate, exencephaly) were observed in fetuses of rats treated during organogenesis with 0.3 and 1.0 mg/kg/day (10 and 47 times the exposure resulting from the maximum recommended human dose based on AUC, respectively). Administration of doses up to 0.3 mg/kg/day Symlin (9 times maximum recommended dose based on AUC) to pregnant rabbits had no adverse effects in embryofetal development; however, animal reproduction studies are not always predictive of human response. Symlin should be used during pregnancy only if it is determined by the healthcare professional that the potential benefit justifies the potential risk to the fetus.

Nursing Mothers

It is unknown whether Symlin is excreted in human milk. Many drugs, including peptide drugs, are excreted in human milk. Therefore, Symlin should be administered to nursing women only if it is determined by the healthcare professional that the potential benefit outweighs the potential risk to the infant.

Pediatric Use

Safety and effectiveness of Symlin in pediatric patients have not been established.

Geriatric Use

Symlin has been studied in patients ranging in age from 15 to 84 years of age, including 539 patients 65 years of age or older. The change in HbA1c values and hypoglycemia frequencies did not differ by age, but greater sensitivity in some older individuals cannot be ruled out. Thus, both Symlin and insulin regimens should be carefully managed to obviate an increased risk of severe hypoglycemia.

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Adverse Reactions

Adverse events (excluding hypoglycemia, discussed below) commonly associated with Symlin when co-administered with a fixed dose of insulin in the long-term, placebo-controlled trials in insulin-using type 2 patients and type 1 patients are presented in Table 4 and Table 5, respectively. The same adverse events were also shown in the open-label clinical practice study, which employed flexible insulin dosing.

Table 4: Treatment-Emergent Adverse Events Occurring With ≥5% Incidence and Greater Incidence With Symlin Compared With Placebo in Long-Term, Placebo-Controlled Trials. Incidence of the Same Events in the Open-Label Clinical Practice Study (Patients With Insulin-Using Type 2 Diabetes, 120 mcg)

 Long-Term, Placebo-Controlled StudiesOpen-Label, Clinical Practice Study
 Placebo + Insulin
(n(%))
(N=284)
Symlin + Insulin
(n(%))
(N=292)
Symlin + Insulin
(n(%))
(N=166)
Nausea 34 (12) 81 (28) 53 (30)
Headache 19 (7) 39 (13) 8 (5)
Anorexia 5 (2) 27 (9) 1 (<1)
Vomiting 12 (4) 24 (8) 13 (7)
Abdominal Pain 19 (7) 23 (8) 3 (2)
Fatigue 11 (4) 20 (7) 5 (3)
Dizziness 11 (4) 17 (6) 3 (2)
Coughing 12 (4) 18 (6) 4 (2)
Pharyngitis 7 (2) 15 (5) 6 (3)

Table 5: Treatment-Emergent Adverse Events Occurring With ≥5% Incidence and Greater Incidence With Symlin Compared to Placebo in Long-Term, Placebo-Controlled Studies. Incidence of the Same Events in the Open-Label Clinical Practice Study (Patients With Type 1 Diabetes, 30 or 60 mcg)

 Long-Term, Placebo-Controlled StudiesOpen-Label, Clinical Practice Study
 Placebo + Insulin (n(%))
(N=538)
Symlin + Insulin (n(%))
(N=716)
Symlin + Insulin (n(%))
(N=265)
Nausea 92 (17) 342 (48) 98 (37)
Anorexia 12 (2) 122 (17) 0 (0)
Inflicted Injury 55 (10) 97 (14) 20 (8)
Vomiting 36 (7) 82 (11) 18 (7)
Arthralgia 27 (5) 51 (7) 6 (2)
Fatigue 22 (4) 51 (7) 12 (4.5)
Allergic Reaction 28 (5) 41 (6) 1 (<1)
Dizziness 21 (4) 34 (5) 5 (2)

Most adverse events were gastrointestinal in nature. In patients with type 2 or type 1 diabetes, the incidence of nausea was higher at the beginning of Symlin treatment and decreased with time in most patients. The incidence and severity of nausea are reduced when Symlin is gradually titrated to the recommended doses (see DOSAGE AND ADMINISTRATION).

Severe Hypoglycemia

Symlin alone (without the concomitant administration of insulin) does not cause hypoglycemia. However, Symlin is indicated as an adjunct treatment in patients who use mealtime insulin therapy and co-administration of Symlin with insulin can increase the risk of insulin-induced hypoglycemia, particularly in patients with type 1 diabetes (see Boxed Warning). The incidence of severe hypoglycemia during the Symlin clinical development program is summarized in Table 6 and Table 7.

Table 6: Incidence and Event Rate of Severe Hypoglycemia in Long-Term, Placebo-Controlled and Open-Label, Clinical Practice Studies in Patients With Insulin-Using Type 2 Diabetes

 Long-Term,
Placebo-Controlled Studies
(No Insulin Dose-Reduction During Initiation)
Open-Label,
Clinical Practice Study
(Insulin Dose-Reduction During Initiation)
 Placebo + InsulinSymlin + InsulinSymlin + Insulin

Severe Hypoglycemia
0-3
Months
(n=284)
>3-6
Months
(n=251)
0-3
Months
(n=292)
>3-6
Months
(n=255)
0-3
Months
(n=166)
>3-6
Months
(n=150)
Patient-Ascertained*
Event Rate (event rate/patient year) 0.24 0.13 0.45 0.39 0.05 0.03
Incidence (%) 2.1 2.4 8.2 4.7 0.6 0.7
Medically Assisted†
Event Rate (event rate/patient year) 0.06 0.07 0.09 0.02 0.05 0.03
Incidence (%) 0.7 1.2 1.7 0.4 0.6 0.7

* Patient-ascertained severe hypoglycemia: Requiring the assistance of another individual (including aid in ingestion of oral carbohydrate); and/or requiring the administration of glucagon injection, intravenous glucose, or other medical intervention.

† Medically assisted severe hypoglycemia: Requiring glucagon, IV glucose, hospitalization, paramedic assistance, emergency room visit, and/or assessed as an SAE by the investigator.

Table 7: Incidence and Event Rate of Severe Hypoglycemia in Long-Term, Placebo-Controlled and Open-Label, Clinical Practice Studies in Patients With Type 1 Diabetes

 Long-Term,
Placebo-Controlled Studies
(No Insulin Dose-Reduction During Initiation)
Open-Label,
Clinical Practice Study
(Insulin Dose-Reduction During Initiation)
 Placebo + InsulinSymlin + InsulinSymlin + Insulin

Severe Hypoglycemia
0-3
Months
(n=538)
>3-6
Months
(n=470)
0-3
Months
(n=716)
>3-6
Months
(n=576)
0-3
Months
(n=265)
>3-6
Months
(n=213)
Patient-Ascertained*
Event Rate (event rate/patient year) 1.33 1.06 1.55 0.82 0.29 0.16
Incidence (%) 10.8 8.7 16.8 11.1 5.7 3.8
Medically Assisted†
Event Rate (event rate/patient year) 0.19 0.24 0.50 0.27 0.10 0.04
Incidence (%) 3.3 4.3 7.3 5.2 2.3 0.9

* Patient-ascertained severe hypoglycemia: Requiring the assistance of another individual (including aid in ingestion of oral carbohydrate); and/or requiring the administration of glucagon injection, intravenous glucose, or other medical intervention.

† Medically assisted severe hypoglycemia: Requiring glucagon, IV glucose, hospitalization, paramedic assistance, emergency room visit, and/or assessed as an SAE by the investigator.

Post Marketing Experience

Since market introduction of Symlin, the following adverse reactions have been reported. Because these events are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure.

General: Injection site reactions.

Overdose

Single 10 mg doses of Symlin (83 times the maximum dose of 120 mcg) were administered to three healthy volunteers. Severe nausea was reported in all three individuals and was associated with vomiting, diarrhea, vasodilatation, and dizziness. No hypoglycemia was reported. Symlin has a short half-life and in the case of overdose, supportive measures are indicated.

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Dosage and Administration

Symlin dosage differs depending on whether the patient has type 2 or type 1 diabetes (see below). When initiating therapy with Symlin, initial insulin dose reduction is required in all patients (both type 2 and type 1) to reduce the risk of insulin-induced hypoglycemia. As this reduction in insulin can lead to glucose elevations, patients should be monitored at regular intervals to assess Symlin tolerability and the effect on blood glucose, so that individualized insulin adjustments can be initiated. If Symlin therapy is discontinued for any reason (e.g., surgery or illnesses), the same initiation protocol should be followed when Symlin therapy is re-instituted (see below).

Initiation of Symlin therapy

Patients With Insulin-Using Type 2 Diabetes

In patients with insulin-using type 2 diabetes, Symlin should be initiated at a dose of 60 mcg and increased to a dose of 120 mcg as tolerated.

Patients should be instructed to:

  • Initiate Symlin at 60 mcg subcutaneously, immediately prior to major meals;
  • Reduce preprandial, rapid-acting or short-acting insulin dosages, including fixed-mix insulins (70/30) by 50%;
  • Monitor blood glucose frequently, including pre- and post-meals and at bedtime;
  • Increase the Symlin dose to 120 mcg when no clinically significant nausea has occurred for 3-7 days. Symlin dose adjustments should be made only as directed by the healthcare professional. If significant nausea persists at the 120 mcg dose, the Symlin dose should be decreased to 60 mcg;
  • Adjust insulin doses to optimize glycemic control once the target dose of Symlin is achieved and nausea (if experienced) has subsided. Insulin dose adjustments should be made only as directed by the healthcare professional;
  • Contact a healthcare professional skilled in the use of insulin to review Symlin and insulin dose adjustments at least once a week until a target dose of Symlin is achieved, Symlin is well-tolerated, and blood glucose concentrations are stable.

Patients With Type 1 Diabetes

In patients with type 1 diabetes, Symlin should be initiated at a dose of 15 mcg and titrated at 15-mcg increments to a maintenance dose of 30 mcg or 60 mcg as tolerated.

Patients should be instructed to:

  • Initiate Symlin at a starting dose of 15 mcg subcutaneously, immediately prior to major meals;
  • Reduce preprandial, rapid-acting or short-acting insulin dosages, including fixed-mix insulins (e.g., 70/30) by 50%;
  • Monitor blood glucose frequently, including pre- and post-meals and at bedtime;
  • Increase the Symlin dose to the next increment (30 mcg, 45 mcg, or 60 mcg) when no clinically significant nausea has occurred for at least 3 days. Symlin dose adjustments should be made only as directed by the healthcare professional. If significant nausea persists at the 45 or 60 mcg dose level, the Symlin dose should be decreased to 30 mcg. If the 30 mcg dose is not tolerated, discontinuation of Symlin therapy should be considered;
  • Adjust insulin doses to optimize glycemic control once the target dose of Symlin is achieved and nausea (if experienced) has subsided. Insulin dose adjustments should be made only as directed by the healthcare professional;
  • Contact a healthcare professional skilled in the use of insulin to review Symlin and insulin dose adjustments at least once a week until a target dose of Symlin is achieved, Symlin is well-tolerated, and blood glucose concentrations are stable.

Once Target Dose of Symlin is Achieved in Type 2 or Type 1 Patients

After a maintenance dose of Symlin is achieved, both insulin-using patients with type 2 diabetes and patients with type 1 diabetes should be instructed to:

  • Adjust insulin doses to optimize glycemic control once the target dose of Symlin is achieved and nausea (if experienced) has subsided. Insulin dose adjustments should be made only as directed by a healthcare professional;
  • Contact a healthcare professional in the event of recurrent nausea or hypoglycemia. An increased frequency of mild to moderate hypoglycemia should be viewed as a warning sign of increased risk for severe hypoglycemia.

Administration

Symlin should be administered subcutaneously immediately prior to each major meal (≥250 kcal or containing ≥30 g of carbohydrate).

Symlin should be at room temperature before injecting to reduce potential injection site reactions. Each Symlin dose should be administered subcutaneously into the abdomen or thigh (administration into the arm is not recommended because of variable absorption). Injection sites should be rotated so that the same site is not used repeatedly. The injection site selected should also be distinct from the site chosen for any concomitant insulin injection.

  • Symlin and insulin should always be administered as separate injections.
  • Symlin should not be mixed with any type of insulin.
  • If a Symlin dose is missed, wait until the next scheduled dose and administer the usual amount.

SymlinPen® pen-injector

The SymlinPen® pen-injector is available in two presentations:

  • SymlinPen® 60 pen-injector for doses of 15 mcg, 30 mcg, 45 mcg, 60 mcg.
  • SymlinPen® 120 pen-injector for doses of 60 mcg and 120 mcg.

See the accompanying Patient Instructions for Use for instructions for using the SymlinPen® pen-injector.

The patient should be advised:

  • to confirm they are using the correct pen-injector that will deliver their prescribed dose;
  • on proper use of the pen-injector, emphasizing how and when to set up a new pen-injector;
  • not to transfer Symlin from the pen-injector to a syringe. Doing so could result in a higher dose than intended, because Symlin in the pen-injector is a higher concentration than Symlin in the Symlin vial;
  • not to share the pen-injector and needles with others;
  • that needles are not included with the pen-injector and must be purchased separately;
  • which needle length and gauge should be used;
  • to use a new needle for each injection.

Symlin vials

To administer Symlin from vials, use a U-100 insulin syringe (preferably a 0.3 mL [0.3 cc] size) for optimal accuracy. If using a syringe calibrated for use with U-100 insulin, use the chart below (Table 8) to measure the microgram dosage in unit increments.

Table 8: Conversion of Symlin Dose to Insulin Unit Equivalents

Dosage Prescribed (mcg)Increment Using a U-100 Syringe (Units)Volume (cc or mL)
15 2 ½ 0.025
30 5 0.05
45 7 ½ 0.075
60 10 0.1
120 20 0.2

Always use separate, new syringes and needles to give Symlin and insulin injections.

Discontinuation of Therapy

Symlin therapy should be discontinued if any of the following occur:

* Recurrent unexplained hypoglycemia that requires medical assistance;
* Persistent clinically significant nausea;
* Noncompliance with self-monitoring of blood glucose concentrations;
* Noncompliance with insulin dose adjustments;
* Noncompliance with scheduled healthcare professional contacts or recommended clinic visits.

Preparation and Handling

Symlin should be inspected visually for particulate matter or discoloration prior to administration whenever the solution and the container permit.

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How Supplied

Symlin is supplied as a sterile injection in the following dosage forms:

  • 1.5 mL disposable multidose SymlinPen® 60 pen-injector containing 1000 mcg/mL pramlintide (as acetate).
  • 2.7 mL disposable multidose SymlinPen® 120 pen-injector containing 1000 mcg/mL pramlintide (as acetate).
  • 5 mL vial, containing 600 mcg/mL pramlintide (as acetate), for use with an insulin syringe.

To administer Symlin from vials, use a U-100 insulin syringe (preferably a 0.3 mL [0.3 cc] size). If using a syringe calibrated for use with U-100 insulin, use the chart (Table 8) in the DOSAGE AND ADMINISTRATION section to measure the microgram dosage in unit increments.

Do not mix Symlin with insulin.

Symlin Injection is available in the following package sizes:

  • SymlinPen® 60 pen-injector, containing 1000 mcg/mL pramlintide (as acetate)
    2 X 1.5 mL disposable multidose pen-injector
    (NDC 66780-115-02)
  • SymlinPen® 120 pen-injector, containing 1000 mcg/mL pramlintide (as acetate)
    2 X 2.7 mL disposable multidose pen-injector
    (NDC 66780-121-02)
  • 5 mL vial, containing 600 mcg/mL pramlintide (as acetate), for use with an insulin syringe
    (NDC 66780-110-01)

Storage

Symlin pen-injectors and vials not in use: Refrigerate (36°F to 46°F; 2°C to 8°C), and protect from light. Do not freeze. Do not use if product has been frozen. Unused Symlin (opened or unopened) should not be used after the expiration (EXP) date printed on the carton and the label.

Symlin pen-injectors and vials in use: After first use, refrigerate or keep at a temperature not greater than 86°F (30°C) for 30 days. Use within 30 days, whether or not refrigerated.

Storage conditions are summarized in Table 9.

Table 9: Storage Conditions

Dosage FormUnopened (not in use)
Refrigerated
Open (in use)
Refrigerated or Temperature
Up To 86°F (30°C)
1.5 mL pen-injector
2.7 mL pen-injector
5 mL vial
Until Expiration Date Use Within 30 days

The SymlinPen® pen-injectors and Symlin vials are manufactured for: Amylin Pharmaceuticals, Inc. San Diego, CA 92121 USA 1-800-349-8919 http://www.Symlin.com

Rx only

The Symlin mark, Symlin design mark, and SymlinPen are registered trademarks of Amylin Pharmaceuticals, Inc. Copyright © 2005-2008, Amylin Pharmaceuticals, Inc. All rights reserved.

Last Updated: July 2008

Symlin, Symlin Pen, pramlintide acetate, patient information (in plain English)


The information in this monograph is not intended to cover all possible uses, directions, precautions, drug interactions or adverse effects. This information is generalized and is not intended as specific medical advice. If you have questions about the medicines you are taking or would like more information, check with your doctor, pharmacist, or nurse.

back to: Browse all Medications for Diabetes

APA Reference
Staff, H. (2008, July 31). Symlin for Treatment of Diabetes - Symlin Full Prescribing Information, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/diabetes/medications/symlin-diabetics-prescribing-information

Last Updated: March 10, 2016

Sunday, June 29, 2008

HI this is test journal entery

APA Reference
(2008, June 29). Sunday, June 29, 2008, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/healthyplace/artical/Sunday%2C-June-29%2C-2008

Last Updated: January 14, 2014

Recognizing Unhealthy Relationships and Creating Healthy Ones

Dr. Kenneth Appel,our guest speaker, is a clinical psychologist who works with individuals, couples and families on relationship issues. Our discussion centered around unhealthy relationships, creating healthy relationships, being in a relationship with someone who has a mental illness, and online relationships.

David Roberts: HealthyPlace.com moderator.

The people in blue are audience members.

David: Good Evening. I'm David Roberts. I'm the moderator for tonight's conference. I want to welcome everyone to HealthyPlace.com. I hope everyone's day has gone well.

Our conference tonight is on "Recognizing Unhealthy Relationships and Creating Healthy Ones". Our guest is Kenneth Appel, Ph.D. Dr. Appel is a clinical psychologist who has worked with individuals, couples, and families for over 37 years. He is on the faculty of the University of California, where he teaches psychiatry residents and also teaches in the Department of Psychiatry at California Pacific Medical Center. I also want to mention that Dr. Appel met his wife online and later tonight we'll talk to him about that and the subject of online relationships.

Good Evening Dr. Appel and welcome to HealthyPlace.com. We appreciate you being here tonight.

So we are all on the same page here, please give us your definition of a "healthy relationship" and an "unhealthy relationship".

Dr. Appel:: A healthy relationship is characterized by dynamic balance and intimacy. An unhealthy relationship is characterized by being severely out of balance, with intimacy diminishing on a rapid curve.

David: "Dynamic balance" means what?

Dr. Appel: Well, consider a picture of the Tai Chi symbol, a circle containing black and white in the form of an OGEE curve. Compare it to the same circle with one half painted black and one half painted white, and you'll see the difference between a relationship with dynamic balance versus one which is static though balanced.

David: Is it hard to find and maintain a healthy relationship?

Dr. Appel: I think not. I think that the opportunity to find healthy relationships is directly correlated with self-knowledge and maturity.

David: A significant number of people seem to hook up with the "wrong person." Why is that? Is it something within ourselves?

Dr. Appel: I think that's a good way to put it, that it might be something within ourselves that's perhaps unconscious, that motivates us to seek out a compliment to something unhealthy in ourselves. So we can learn from relationships like this and learn more about ourselves perhaps than about the other.

David: I'm also thinking that sometimes we meet a person, develop a relationship with them, then after several years, it all seems to fall apart. It used to be that when a person considered marriage, that it would be forever. That's no longer true. Do you think that it's extremely difficult to have a satisfying long-term love relationship?

Dr. Appel:: The nature of marriage seems to be changing parallel to the extension of life span. That is, as we have many many more years to live, the notion of "till death do us part" is being defied by current sociological evidence about divorce. However, there are many relationships which follow a developmental course, that last indeed forever and remain in dynamic balance, share intimacy, and continue to grow.

David: What is the criteria one should use to decide this is an "unhealthy relationship?"

Dr. Appel: There will be gut feelings that will inform you that "something is wrong." These feelings should be trusted. As they are trusted, they will begin to clarify what is going wrong in the relationship. For instance, diminishing intimacy, lack of sex, which usually begins with the distaste for kissing, fewer common goals. But above all, what you will feel is a closing of the heart, and everything in the relationship is then open to criticism.

David: The reason I asked that question is that, as you know, we are a mental health community here at HealthyPlace.com. I get letters all the time from visitors and one topic that comes up a lot is how difficult it is to maintain a relationship when either you or your partner, have a psychiatric disorder. As you can imagine, there can be some very trying times. I would like you to address that subject and give us some insight into when, or if, the non-ill partner should say "I'm getting out."

Dr. Appel: Good question. In the presence of a severe psychiatric disorder, that is one that is clinically manifested, relationships are severely stressed, and it is natural for the non-ill partner to wish to be out of the relationship and at the same time not to abandon the partner who is in trouble. The more severe the illness, the greater the stress on the relationship. And here, I'm talking about uncontrolled bipolar disorder, untreated psychotic depression, severe obsessive-compulsive disorder, agoraphobia, etc.


On the other hand, there are conditions known as borderline conditions (for instance, Borderline Personality Disorder, BPD) in which the partner who is ill is always in a very strong or avoidant position, making them very difficult to live with.

In less severe disorders, minor personality problems, transient depressions, relationships are less stressed, and consequently more easily maintained. But the real answer that people are seeking, is about when to leave. And I think that one has to get professional help to make this decision and to look for points where they can no longer contain the illness and are beginning to be symptomatic themselves. That's clearly time to think about leaving.

David: We have a lot of audience questions. Here's one that deals with what we are talking about now:

Kirsten700: I am currently separated (husband's choice) and am trying to figure out if my marriage is worth saving. Husband refuses to go to counseling, he thinks he can work out his 'issues' on his own. Should I bother or should I walk away? I get the feeling he still loves me but has some childhood things he needs to deal with. I just don't know if he will. And if he won't, is it worth it for me to stay??

Dr. Appel: You've hit the nail right on the head. He probably does have some childhood issues that he has to deal with, and it's natural to want to know whether you should wait while he goes through that or get on with your life. That he will not seek help to work these through is an indicator of a strong need for independence and autonomy, as well as an avoidance of what could be talked about and resolved in counseling, if he really wanted to. My guess is, that if he doesn't go to treatment, that he will not work them out on his own, and that you might profit by a couple of counseling sessions investigating the question, "What's keeping me in there?"

cindydee: I am borderline. Do you think two borderlines can have a healthy relationship?

Dr. Appel: I would have to know how you define "borderline", but when I think of the defenses of borderline, such as things are all good or all bad, not being able to integrate themselves or others as whole people, I would think that it would be very difficult for two borderlines, who actually fit the diagnostic criteria, to have a relationship which is in dynamic balance and intimate. Withdrawal of love, and lack of object constancy make relationships between borderlines extremely difficult, though exciting.

waterfall: What if I have Bipolar Disorder, Manic Depression and it was triggered by the failure to maintain a much-needed relationship and the partner was the one to blame. I asked him to come with me to get help and he refused. Now I've been through two manic episodes and more alone than when I was in the relationship with him. What do I do now? Thanks

Dr. Appel: Bipolar disorder is a neurophysiological problem which can be dealt with through the use of mood stabilizers, anti-depressants, and psychotherapy. Though the loss of the relationship might have been coincident with your first episode, it would be off the mark to say that a relationship, or the end of the relationship, was responsible for the bipolar disorder.

My suggestion is to get appropriate treatment, and when you are feeling more self-confident, to seek another relationship.

rwilky: Hi Dr. Appel. I have personally found that I had to get my life in order and become responsible for myself, and know myself to find a better relationship. That caused me to stop looking for "cheap thrills" and find someone that is already more stable and that has her life in order. That has helped me to have a more peaceful and stable life, and helped me take charge of my own life. What I am asking is, can't people benefit more from selectively "weeding out" poor candidates and finding people that are more stable themselves?

Dr. Appel: Good for you! Not only will it benefit individual relationships, but in the end, it will benefit the gene pool if people begin by selecting mates who have qualities of mental health and physical health that are at least equal to, or somewhat above, their own level. To put it in your terms, someone who is more stable can certainly help another to grow and to move to a position of stable mental health themselves. In terms of weeding out candidates, it seems to me that's the whole job one begins in adolescence, and continues on to some level where they can find a mate with whom they can be in a dynamically balanced relationship.

David: As I'm reading your responses, I'm thinking to myself, would you suggest to almost every person that they go into therapy yourself BEFORE you start looking for a mate or, at least, before you get married?

Dr. Appel: Absolutely not. I would stay as far away from therapy as I could if I felt self-confident, alert, and socially mobile. I would not recommend premarital therapy because there is a natural developmental course that we all follow, which will eventually lead us to a suitable mate.

David: Before we move on, I also want to touch on the subject of single parenthood and how difficult it must be to have children who suffer from a mental disorder and then trying to find a partner. In fact, here's an audience question on that subject, then I'll ask my questions.


ksisil: As a single parent of a special needs child, how would you even go about having a relationship. I mean if it doesn't work, then my child is suffering, or his disorders scare most men off.

Dr. Appel: It is difficult enough to find a relationship for a single parent period. Having a child with special needs makes this difficult, and would take someone with a really open heart, and a soulmate love for you, to move into this situation. I wish I could more clearly answer this question for you. I imagine this particular dilemma could be approached through online dating, which we'll be talking about soon.

David: One question I had was, as a parent, when can I put my "needs" forward as a priority? Needs for friendship, companionship, love, sex?

Dr. Appel: As a parent in a married relationship, the needs between the couple and the children are constantly changing and in flux. But the idea of dynamic balance should be kept in mind. As a single parent, that juncture will also depend on the age and stage of development of the child. The timing has to accord to the growth of both the parent and the child. If it is driven on the part of the adult, the timing is probably inappropriate. If it feels natural and agreeable, follow your feelings.

Jack_39: I have found someone that I love very deeply and she loves me as well. Unfortunately she is still married because she is afraid of hurting her young children. It has been over a year and we do love each other so much. What can I do? Should I let her go or wait?

Dr. Appel: Tough situation. If you love this person as deeply as you can, then you will take into consideration her need not to hurt her children. As a mother she knows more about this than anyone else. Respect her decision, and in terms of waiting, you will have to find time to go on with your life, and see if your feelings for her endure. And if your feelings prohibit you from forming other relationships as well. Sometimes we just have to back away from what seems wonderful, and let it play out in order to understand its lesson.

richcos: Dr. Appel: My wife, 34 years old, suffers from rapid cycling bipolar disorder. She takes all her meds, has an excellent physician, but she hasn't been herself for years. What can you recommend to the spouse in terms of coping skills, etc.

Dr. Appel: First coping skill: seek someone to talk to about it. It doesn't have to be a therapist. It could be clergy, or someone trained in listening. If she hasn't been herself in years, then you haven't been yourself in years either. So it's necessary to be that self, and to discover ways to cope while staying and ways to deal with the rapid cycling. I can only imagine it's extremely difficult for both of you.

David: I'd be interested in getting some audience comments. Maybe we can help each other here. If you are in a relationship with someone who has a mental illness, how are you making it work? For those who have asked, here's the link to the HealthyPlace.com Relationships Community. You can click on this link to sign up for the mail list at the top of the page so you can keep up with events.

Beverly Russell: I just got out of a relationship with someone who was diagnosed with obsessive compulsive personality disorder. What do you know about this disorder and how does it effect relationships.

Dr. Appel: Obsessive compulsive disorder, depending on its severity, can impact relationship in devastating ways. For the person with the disorder, control is everything. The major characteristic is the attempt on the patient's part to hold the world still while obsessing about problems of safety, contamination, etc. Or they may have repetitive ritual activities. All take the attention not only of the ill person, but of anyone living with him or her. I remember my mother saying some hundred miles into a trip, "did I turn the gas off? or did I lock the door?" She had a mild form of the illness. My father didn't turn around under her control and go back. But in the severe form of the illness where a person has say a compulsive hand-washing ritual, a severe fear of contamination, not only holds the world still, but shrinks it for himself and those around him or her.

David: Here are some audience responses to "how you are making it work - being in a relationship with someone who has a mental illness:"

catino: I have been married for over 25 years to the same person and just recently found out that she has MPD (Multiple Personality Disorder). We have been trying to work on our relationship but it is and has been a very difficult time for the past few years. I love her with all my heart and really want to work through all the problems and get our relationship back in harmony.

PEBBLES2872: Mental illness is 95% perception based on what one expects from someone else, and as time goes on, one finds out that they are not living up to your expectations.

David: Here's the flip side of the coin, Dr. Appel. How would you respond to this person:

Joni: I suffer from bipolar disorder, and I feel a burden to my mate. I'm separated and have met and love someone else - and he's "the one". I feel like a burden to him too.


Dr. Appel: This should be handled in your therapy. And that is a real therapeutic issue. Feeling a burden to someone seems to be a part of the depressive side of the illness or disorder. I think you should talk to your therapist about this.

brooke1: Joni, maybe you should believe him if he says you are not a burden.

David: Here's another audience comment from someone who had Borderline Personality Disorder:

sweetpea1988: Hello, I was married for 8 years and I have borderline personality disorder. He tried to keep me from getting better, he loved the control he had over me. Two years ago, I finally left him. I took our three daughters with me, but lost them due to my illness, but now I have learned a lot and I am on my own. I feel much better about myself and life itself. I have hurt myself for 16 years and now since I left him I have stopped.

David: As I mentioned earlier, Dr. Appel married a woman that he met online. People are doing this more-and-more these days--finding relationships online. Can you share a bit of your story with us Dr. Appel?

Dr. Appel: I'd be glad to. I was in San Francisco on Valentine's Day in 1997, and a promotional ad came in my email from One-and-only.com to place a free ad on their dating service. I immediately deleted it and went on with what I was doing. But then I had second thoughts and placed an ad describing myself and the kind of relationship I wanted. On April 18, I got an answer from Beverly. And that was the beginning of an email correspondence which numbered well over 1000 pages in two months. Beverly was in Tennessee, and our phone bills became enormous. And because our love had developed during this, we decided to meet in June in San Francisco. Everything we had learned about each other online/phone turned out to be wonderful and true. We have been together since that time, and truly feel we are soulmates. Out of this experience and correspondence and interviews with hundreds of people, we wrote "It Takes Two.Com," A Psychological and Spiritual Guide to Finding Love on the Internet Personals, in the hope that we could illustrate to others that good healthy relationship was possible on the Net, and that meeting from the inside-out could bring one closer than meeting in person.

David: We have some more audience suggestions on how to deal effectively in a relationship with someone who has a mental illness. I want to post those, and then we'll continue:

richcos: Serious mental illness in a marriage is tough, no doubt about it. Make sure you've found the best possible psychiatrist for your loved one. And then a therapist for yourself to make sure that you remain mentally ok. It's often unremitting stress and I would suggest looking at the spiritual angle for guidance. It's not easy, but if you can meet the challenge, you can feel a real sense of accomplishment that you didn't run away from the person you love.

Dr. Appel: richcos, I think this is a wonderful comment, and I am so glad to hear you say that the spiritual side will often help you through this dilemma, and enable you to stay with your loved one, and essentially see the relationship as a devotion without becoming martyred.

David: That is a wonderful story Dr. Appel. Commonality, of course, brings people together. And especially now, with the internet, many people with mental illness are meeting up and discovering they are not out there alone. Is this a good way to meet people?

Dr. Appel: It's going to depend on individuals, just like meeting each other face-to-face. The main thing is to be yourself, be honest, be mindful, and follow your feelings and intuition. The more you know from email, the more possible it is to make the right decision.

David: Do you think communicating via email is better, initially, than chatting?

Dr. Appel: Often it can be. It seems to give one a greater sense of distance and time to think about what they're feeling and saying. Chats often have the feeling of demand that you might find in a singles bar.

David: Here are some more audience responses to what's been said tonight:

bcooper: My boyfriend is having a hard time living with me. I have obsessive compulsive disorder (ocd) and panic.

Beverly Russell: My self-esteem has suffered a great deal as well as my self-confidence. I left because he no longer was interested in me and would not even speak or look at me when I informed him I was leaving. I have been thinking about therapy.

Jocasta: What are the chances/statistics of two people in a commitment (6+ yrs.) who both have mental disorders staying together in your experience with working with couples? Would you advise of a specific way for one party to convince the other that they need medication when that party is adamant about not taking any? And, can one party develop systems of the other's disorder from being attached for so long (codependence?) with very few friends?


Dr. Appel: This is a really complicated question. The only thing I can say here is something often said in AA and other 12 step programs: It is imperative to take your own inventory. It is imperative not to take the inventory of others.

SkzDaLimit: I am currently engaged to a wonderful woman who is diagnosed Bipolar I (rapid cycler). The problem I have is she does have occasional fits of anger, and she seems to draw me into lashing out in anger towards her. Are there any suggestions as to how I might deal with this?

Dr. Appel: This is a common situation in rapid cycling rage--that the partner is often drawn in. It is almost as if the partner takes on the rage of the bipolar. The only way to deal with it is to step away from it, even though this arouses more rage in the bipolar partner. The other solution is to "teflonize" yourself, that is, to contain the rage without absorbing it.

samantha 1: Do you think that codependence is a major problem in relationships?

Dr. Appel: I'm never sure what co-dependency really is. What I do know is that interdependence is a feature of healthy relationships. Co-dependence seems to be so enmeshed that often the sense of who is who is lost.

Sarah4: Is it possible to be in a relationship, break it off, and find that you have become better friends, more in tune to each other after, and if so, would you suggest trying it again?

Dr. Appel: It's absolutely possible, and I would suggest that you remain good friends. Natural development will take care of the rest. The less you think about it and the more you experience it, the more you will learn.

Dr. Appel: Also, Beverly has just written a new book, A Guide to Online Dating, which can be found at http://dlsijpress.com. It's an e-book, and also available for the sight impaired.ACMercker: Dr. Appel, how does one deal with infidelity on the part of their ill partner? My patience seems to be both a strength and a flaw.

Dr. Appel: If the infidelity is part of the illness, as it often is in hypomania, then one should understand it as such. If it's part of the pull out of the relationship, the only way to deal with it is through therapy or through a very strong spiritual approach. There is no understanding of repetitive infidelity. What I mean is that understanding will get you nowhere. Repetitive infidelity means the other person isn't in the relationship anymore, and you shouldn't be either. Even if it's manic acting out.

catino: I agree with ACMercker about patience.

David: Somehow, after awhile, even if you're a "saint," and maybe this is just my perspective, but "understanding" repetitive infidelity would be tough. Here's an important question on adolescent relationships:

ksisil: This may be a little off the topic but in terms of adolescent relationships, how can I encourage these with my son when any child who has seen his rage never wants to come around again and of course when he calms down he is broken hearted because no one will play with him.

Dr. Appel: There are groups in larger cities and at university centers dealing with the problems of adolescents such as you describe. In these groups, they learn relationship skills under techniques of cognitive behavioral therapy. They are quite successful, and you might be able to find groups like this online.

David: What about creating healthy relationships? When people say that, it sounds easy. "We just all get along." What are the keys to having a healthy relationship?

Dr. Appel: The key to a healthy relationship is that it is developmental in nature, many have beginnings and ends, and some last a lifetime. To create a healthy relationship, the main key is to give up judgment. This is extremely difficult. But if one can talk in "I" statements and not be judgmental and critical, relationships will endure. And, of course, as they develop, the development is deeper and stronger. It is not an answer to the wish, "I wish it was like it was at the beginning."

David: And intimacy takes effort, isn't that right Dr. Appel?

Dr. Appel: Absolutely. And once the effort is expended, it is so easy!

Jessica Neal: A year-and-a-half ago, I was diagnosed with bipolar disorder after having about 3-4 months of rapid-cycling episodes. During those episodes I said a lot of hurtful sexual remarks to my husband. Some I remember saying, some not. I'm wondering what can I do to help alleviate his pain? It was hard enough for me to deal with bipolar, but now we have this hanging over our heads.

Dr. Appel: He should get some help to understand that those remarks were made in the heat of mania. And even though you might feel them deeply to be true, he will still have to deal with the hurt in treatment. Now that you have your illness under control, you'll be able to begin to be complimentary in a way that will rebuild his sexual self-esteem.

catino: Why is it that people find it so hard to decide that they may need therapy? How do they know that they do, in fact, need it?

Dr. Appel: If one is thinking about it, then perhaps there are some problems alive that need attention. If the person feels that a lot of their energy is tied up in conflict, such as difficulties with authority, relationships, aggression, and other symptoms, then the time has come to seek therapy. If you sense these symptoms coming on, therapy might help to preempt them.

David: It is getting late. I want to thank Dr. Appel for being our guest tonight and for sharing his insights and knowledge with us.

I also want to thank everyone in the audience for coming tonight and participating. That's what makes these conferences so wonderful and informative.

Dr. Appel: Thank you for inviting me! I think you have a wonderful community here. It's been stimulating to talk with you.

David: Good night, Dr. Appel. And good night everyone.

APA Reference
Staff, H. (2008, June 17). Recognizing Unhealthy Relationships and Creating Healthy Ones, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/relationships/transcripts/recognizing-unhealthy-relationships-and-creating-healthy-ones-online-conference-transcript

Last Updated: June 8, 2019

Infidelity: Cheating in Your Relationships

Elissa Gough

Elissa Gough, has experienced the addictiveness and excitement that affairs have to offer, as well as the turmoil. She joined us to answer your questions about infidelity and how to deal with cheating in your relationships. She also discussed when and when not to tell your partner about the "other woman" or "other man," same-sex affairs, and emotional infidelity.

David Roberts: HealthyPlace.com moderator.

The people in blue are audience members.


David: Good Evening. I'm David Roberts. I'm the moderator for tonight's conference. I want to welcome everyone to HealthyPlace.com. I'm glad you had the opportunity to join us and I hope your day went well. Our topic tonight is "Infidelity." Our guest is author and coach Elissa Gough.

Our topic tonight is "Infidelity: Cheating In Your Relationships." For 30 years, Elissa Gough was an emotional hostage, unwilling to free herself from relationships which caused her great pain. She shared her story and insights in her book, Infidelity. Tonight, we will be talking with her about how to manage the passion and pain of affairs.

Ms. Gough will share proven ways of coping with betrayal for everyone affected - spouses, partners, children, other family members, the "other man or other woman," gay men and lesbians - with an emphasis on individual responsibility, accountability and commitment, and with the overall objective of keeping marriages whole and/or relationships healthy.

Good evening, Elissa, and welcome to HealthyPlace.com. Thank you for joining us tonight. Maybe it's a good thing to start off with your definition of "infidelity."

Elissa Gough: I am happy to be here, thanks. Infidelity means different things to different people. I believe that any emotion or act that takes you away from your exclusive bond with your spouse or partner is an act of infidelity. Infidelity is not just physical. In fact, sex does not have to be a factor.

David: Then, it can be an emotional bond, also?

Elissa Gough: Yes, in fact, emotional infidelity can be much more damaging to a relationship than physical. Emotional bonds can be more devastating to a betrayed spouse because it creates a connection that's hard to break. Having your spouse love someone else is more painful than having your spouse just "fool around."

David: In my introduction, I mentioned that you had a long history of unhealthy relationships. How did you get caught up in the cycle of infidelity?

Elissa Gough: My first affair came about due to a tragedy. My daughter had leukemia and I became emotionally involved with her doctor. I thought he could save her; he became very close to my family. I felt very dependent on him. Marriages became a cycle for me. I was looking to recreate a family that I had lost. I had lost both my father and child very early in life.

David: I know many people have affairs. I'm wondering, in your opinion, is it psychologically easy for people who are in committed relationships to have affairs?

Elissa Gough: It's not easy. Some affairs are situational, some are just one time flings, while others make a lifetime career out of cheating. They are heart-wrenching to everyone involved. They drain you.

They are exciting and they're addictive. It's the excitement and the passion that draws you and keeps you entangled in the web. Once you're in, you justify and find reasons to keep it going. It becomes a "fix" for some. You rationalize and avoid the pain it causes.

David: So everyone in the audience knows where you are coming from, do you feel that affairs are wrong?

Elissa Gough: After my years of experience, I don't condone affairs, but I understand how they are born, live, and how they die. I try not to moralize, analyze, or judge. I am just here to provide information and spread awareness. We want to knock down the walls of shame and embarrassment so those involved can face their reality. This is a topic that has been ignored, and when it is talked about, it is exploited. Those who suffer the pains of infidelity are left with nowhere to go.

David: I want to address this topic from two sides:

  1. The person having the affair
  2. The other is the person who we might call "the victim," the one left behind.

One of the first things I always see come up -- should the person having the affair tell his/her partner about it if they don't know about it?

Elissa Gough: It depends on the situation. There are many variables. Will the spouse be able to handle it, etc? Professional help should be sought prior to making any decisions like that. There are so many variables, there's no clear cut answer.


David: Maybe we can tackle that question another way. What would be the benefit to the other person, the victim, to being told about the affair?

Elissa Gough: I don't really like the word "victim." Victim means someone is helpless. I like to teach people to be proactive and not let themselves be victimized. Sometimes there is no benefit. The benefit of knowing leads to change, whether there's a divorce or it leads to a stronger marriage there can be benefits. And sharing it can break the cycle.

David: We have an audience comment about what's been said so far, then we will get into some of the audience questions.

Lauren1: I am not proud to say that I have had three affairs in the past 4 1/2 years. As Elissa said, they drain you because it is exhausting living a "double life." There is so much guilt when you are with your spouse, not to mention the "covering up" of the time that you are with the person with whom you are having the affair. Let me add, please, that it may seem exciting at the time you are with the person, but then when you depart, it is an awful pain of emptiness, unfulfillment, and feeling "dirty."

David: Here's the first question:

bossy: I had an affair last year and I decided that it would be way too hurtful for my husband to know about it. I am very, very regretful and angered that I had the affair myself. I sometimes wonder, "If I tell my husband will it alleviate my anger?" That kinda sounds selfish.

Elissa Gough: Exactly, you need to be very careful. I suggest that you focus on breaking your cycle of infidelity. Devote time to self-discovery so you can find out why you had your affair so that your can prevent it from happening again. Telling the truth can be difficult; it's a choice you have to make on your own. I can only tell you the consequences.

David: That's what I was getting at earlier, Elissa. The person having the affair gets to relieve him/herself of some of the guilt, and I'm wondering what the person who learns about the affairs gets out of it besides a lot of pain.

Elissa Gough: Exactly, if telling the truth is just about relieving your own guilt and now helping further your relationship, then maybe it might be better left unsaid.

sanders: Same-sex affairs seem less of a betrayal than opposite-sex affairs! Is that a common thought or just a justification for homosexual or lesbian behavior?

Elissa Gough: I think it's a justification. It relieves one's guilt and rationalizes deception. As I said earlier, anything that breaks the exclusive bond of a committed relationship is a betrayal.

Burntsoul: I was with a man who was having an affair with his wife. I didn't know it until afterward because he lied to me. Why would he tell me he loved me in front of his wife?

Elissa Gough: I am not sure I understand the question fully. He was having an affair with his wife?

Burntsoul: He was having an affair with me, and I ended up meeting his wife and he told me he loved me in front of her, and it was more than once.

Elissa Gough: Well, he may love you, but he also loved her at one time as well. I think that shows how little respect he has for his wife, which may be you someday. Remember, patterns are difficult to change, even if he changes partners.

David: And that's a good point Elissa. Would you say that for most people, "once a cheater, always a cheater?" Many people hold out hope that the person will leave his/her spouse. Is that realistic? And secondly, when one thinks about it, if this person cheated on his/her spouse or partner, why wouldn't he/she do that to you?

Elissa Gough: People can modify their behavior if they want to. I am a great example of how someone can change. "Once a cheater, always a cheater" is stereotypic. It is true that people do have patterns of behavior and if they aren't willing to change, the pattern will continue. There has to be a desire to change. No one can change a person, or their behavior. You had a good point. The fact that your lover cheated on his/her spouse should be a wake up call to you. It could to happen to you as well. You are not exempt from being betrayed.

David: If you are the other spouse or partner, what are your suggestions for handling and coping with news that your partner has been cheating on you?

Elissa Gough: It is one of the most devastating things that can happen to someone. They need to try to remain quiet and calm. Don't make rash decisions based on anger or vengeance. Do not run to an attorney or make threats or ultimatums.


Stay focused on taking care of yourself. Take time and sort it out. I know this sounds difficult. That's why an outside support system is needed. Face Reality is a strong advocate for therapy from someone you trust and feel comfortable, whether it be a psychologist or a member of the clergy. Avoid being impulsive.

David: Here's the next question:

abby_normal: I found out in November that my husband was having a two-year relationship. Since we've been trying to reconcile, I found out 3 days ago that he's been lying and deceiving me about her all over again. Now he's claiming insanity. I really don't know what to do. He continues to work with this woman.

Elissa Gough: First, refocus on yourself. Intervene on your own behalf. It's time you take action for yourself. I have been where you've been; I know how hard it is to stay focused. I really advocate support groups because they surround you with others in your situation. Until Face Reality, there were no support groups regarding this topic. It's definitely easier to face this with support behind you.

Don't act impulsively. Think about the consequences of any actions you are considering. If you have children, always keep them in mind.

abby_normal: I found everything out from this woman and my husband corroborated it all, but only when absolutely confronted by all the information. I told him I would postpone any drastic measures on my part until he gets help, but I am going to let him know that I am not going to postpone my life any longer and am going to do whatever I need to find happiness right now. What do you think?

Elissa Gough: It sounds like you are on the right track. Only after you've resolved this situation can you find real peace.

David: I imagine the hardest part of trying to repair a relationship that's been hurt by cheating is the trust. How do you learn to trust this person again?

Elissa Gough: It's very difficult. Once the breach of trust has been broken, it can be mended. It is easier to rekindle love than it is to rebuild trust. Building self-esteem and self-confidence will lead to being able to trust again. You must trust yourself and your own judgment before you can trust others.

David: Here's another audience comment:

Lauren1: If my husband found out about my affairs, he would ask me questions about every single detail. This would be extremely painful for both of us. Last April I had so much guilt that I tried to take my life. Now my husband and I are separated and I just had another affair!! My therapist is helping me, however, to change my selfish, self-destructive behavior.

bossy: You said in your first statement that you believe affairs are any emotional bond that draws you away. That must be a hard line to draw since often having a good time with another male, other than my husband, really gives me a good feeling. Even seeing my psychiatrist each week makes me feel good. If he occasionally shakes my hand or puts his hand on my shoulder it makes me feel good. Is that what you mean?

Elissa Gough: When you dwell on those feelings, fantasize that they will happen again, or desire to be near that person, that's a red flag. Affairs can start out innocently. Men and women can be friends, but it is a dangerous path when you find yourself wanting more.

David: Thank you, Elissa, for being our guest tonight and for sharing this information with us. And to those in the audience, thank you for coming and participating. I hope you found it helpful. We have a very large and active community here at HealthyPlace.com. You will always find people in the chatrooms and interacting with various sites.

I invite everyone to stay and chat in any of the other rooms on the site. Also, if you found our site beneficial, I hope you'll pass our URL around to your friends, mail list buddies, and others. http://www.healthyplace.com

Thanks again, Elissa, for coming tonight.

Elissa Gough: Thank you so much for having me as a guest. I hope the information I provided was helpful.

David: It was. Good night everyone.


Disclaimer: We are not recommending or endorsing any of the suggestions of our guest. In fact, we strongly encourage you to talk over any therapies, remedies or suggestions with your doctor BEFORE you implement them or make any changes in your treatment.

 

APA Reference
Staff, H. (2008, June 17). Infidelity: Cheating in Your Relationships , HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/relationships/transcripts/infidelity-cheating-in-your-relationships-online-conference-transcript

Last Updated: June 8, 2019

Relationships Conference Transcripts

APA Reference
Staff, H. (2008, June 16). Relationships Conference Transcripts, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/relationships/transcripts/relationships-conference-transcripts

Last Updated: August 8, 2014

Glyset Diabetes Type 2 Treatment - Glyset Patient Information

Brand Names: Glyset
Generic Name: miglitol

Pronounced: (MIG lih tall)

Glyset, miglitol, full prescribing information 

What is Glyset and why is miglitol prescribed?

Miglitol delays the digestion of carbohydrates (forms of sugar) in your body. This decreases the amount of sugar that passes into your blood after a meal and prevents periods of hyperglycemia (high blood sugar).

Miglitol is used to treat non-insulin-dependent (Type II) diabetes mellitus.

Miglitol may also be used for purposes other than those listed in this medication guide.

What is the most important information I should know about miglitol?

Take each dose of miglitol with the first bite of a main meal.

Know the signs and symptoms of low blood sugar, which include headache, drowsiness, weakness, dizziness, fast heartbeat, sweating, tremor, and, nausea. Carry glucose tablets, paste, or another glucose or dextrose substance to treat episodes of low blood sugar.

Who should not take miglitol?

Before taking this medication, tell your doctor if you have

  • an inflammatory bowel disease, such as ulcerative colitis or Chron's disease; or any other disease of the stomach or intestines;
  • ulcers of the colon;
  • a blockage or obstruction in your intestines; or
  • kidney disease.

You may not be able to take miglitol, or you may require a dosage adjustment or special monitoring during treatment if you have any of the conditions listed above.

Call your doctor if you develop a fever or an infection, or if you experience a serious injury. You may require insulin for a period of time to control your blood sugar levels.

Miglitol is in the FDA pregnancy category B. This means that it is not expected to harm an unborn baby. Do not take miglitol without first talking to your doctor if you are pregnant. Miglitol passes into breast milk and may affect a nursing infant. Do not take miglitol without first talking to your doctor if you are breast-feeding a baby.


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How should I take miglitol?

Take miglitol exactly as directed by your doctor. If you do not understand these directions, ask your pharmacist, nurse, or doctor to explain them to you.

Take each dose with a full glass of water. Take each dose with the first bite of a main meal. Store miglitol at room temperature away from moisture and heat.

What happens if I miss a dose?

Take the missed dose as soon as you remember. However, if it is almost time for your next dose, skip the missed dose and take only your next regularly scheduled dose. Do not take a double dose of this medication.

What happens if I overdose?

Seek emergency medical attention.

An overdose of this medication is unlikely to occur. Symptoms of an overdose are unknown, but stomach pain, gas, bloating, and diarrhea might be expected.

What should I avoid while taking miglitol?

Follow your doctor's diet and exercise recommendations to help control your blood sugar levels.

Use alcohol cautiously. Alcohol may affect your blood sugar levels.

Miglitol side effects

Stop taking miglitol and seek emergency medical attention if you experience an allergic reaction (difficulty breathing; closing of your throat; swelling of your lips, tongue, or face; or hives).

Other, less serious side effects, are more likely to occur. Continue to take miglitol and talk to your doctor if you experience

  • abdominal pain,
  • diarrhea,
  • flatulence, or
  • a rash.

Side effects other than those listed here may also occur. Talk to your doctor about any side effect that seems unusual or that is especially bothersome. You may report side effects to FDA at 1-800-FDA-1088.

Miglitol Dosing Information

Usual Adult Dose for Diabetes Mellitus Type II:

Initial dose: 25 mg orally 3 times a day at the beginning (with the first bite) of each meal.

What other drugs will affect miglitol?

Digestive-enzyme supplements such as pancreatin (amylase, protease, lipase) in products such as Arco-Lase, Cotazym, Donnazyme, Pancrease, Creon, Ku-Zyme, and others may decrease the effects of miglitol. These medications should not be taken at the same time as miglitol.

Before taking this medication, tell your doctor if you are taking any of the following medicines:

  • propranolol (Inderal);
  • ranitidine (Zantac, Zantac 75);
  • digoxin (Lanoxin, Lanoxicaps),
  • another diabetes medicine such as glyburide (Micronase, Diabeta, Glynase), glipizide (Glucotrol), tolbutamide (Orinase), metformin (Glucophage), and others;
  • a thiazide diuretic (water pill) such as hydrochlorothiazide (HCTZ, Hydrodiuril, others), chlorothiazide (Diuril), chlorthalidone (Thalitone), indapamide (Lozol), and others;
  • a steroid medication such as prednisone (Deltasone), methylprednisolone (Medrol), and others;
  • an estrogen (Premarin, Ogen, and others) or an estrogen-containing birth control pill;
  • a thyroid medication (Synthroid, Levoxyl, and others);
  • phenytoin (Dilantin); or
  • a calcium channel blocker such as verapamil (Calan, Verelan, Isoptin), diltiazem (Cardizem, Dilacor XR), nifedipine (Procardia, Adalat), and others.

The drugs listed above may interact with miglitol or affect blood sugar levels. You may require a dosage adjustment or special monitoring during treatment if you are taking any of the medicines listed above.

Drugs other than those listed here may also interact with miglitol or affect your condition. Talk to your doctor and pharmacist before taking any prescription or over-the-counter medicines.

Where can I get more information?

  • Your pharmacist has more information about miglitol written for health professionals that you may read.
  • Remember, keep this and all other medicines out of the reach of children, never share your medicines with others, and use this medication only for the indication prescribed.

last updated 05/2008

Glyset, miglitol, full prescribing information

Detailed Info on Signs, Symptoms, Causes, Treatments of Diabetes

back to: Browse all Medications for Diabetes

APA Reference
Staff, H. (2008, May 30). Glyset Diabetes Type 2 Treatment - Glyset Patient Information, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/diabetes/medications/glyset-type-2-diabetes-treatment

Last Updated: July 21, 2014

Glyset for Treatment of Diabetes - Glyset Full Prescribing Information

Brand Name: Glyset
Generic Name: Miglitol

Contents:

Description 
Clinical Pharmacology
Clinical Studies
Indications and Usage
Contraindications
Precautions
Adverse Reactions
Overdosage
Dosage and Administration
How is Supplied

Glyset, miglitol, patient information (in plain English)

Description

GLYSET Tablets contain miglitol, an oral alpha-glucosidase inhibitor for use in the management of non-insulin-dependent diabetes mellitus (NIDDM). Miglitol is a desoxynojirimycin derivative, and is chemically known as 3,4,5-piperidinetriol, 1-(2-hydroxyethyl)-2-(hydroxymethyl)-, [2R-(2α,3β,4α, 5β)]-. It is a white to pale-yellow powder with a molecular weight of 207.2. Miglitol is soluble in water and has a pKa of 5.9. Its empirical formula is C8H17NO5 and its chemical structure is as follows:

Miglitol Chemical Structure

GLYSET is available as 25 mg, 50 mg and 100 mg tablets for oral use. The inactive ingredients are starch, microcrystalline cellulose, magnesium stearate, hypromellose, polyethylene glycol, titanium dioxide, and polysorbate 80.

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Clinical Pharmacology

Miglitol is a desoxynojirimycin derivative that delays the digestion of ingested carbohydrates, thereby resulting in a smaller rise in blood glucose concentration following meals. As a consequence of plasma glucose reduction, GLYSET Tablets reduce levels of glycosylated hemoglobin in patients with Type II (non-insulin-dependent) diabetes mellitus. Systemic nonenzymatic protein glycosylation, as reflected by levels of glycosylated hemoglobin, is a function of average blood glucose concentration over time.

Mechanism of Action

In contrast to sulfonylureas, GLYSET does not enhance insulin secretion. The antihyperglycemic action of miglitol results from a reversible inhibition of membrane-bound intestinal α-glucoside hydrolase enzymes. Membrane-bound intestinal α-glucosidases hydrolyze oligosaccharides and disaccharides to glucose and other monosaccharides in the brush border of the small intestine. In diabetic patients, this enzyme inhibition results in delayed glucose absorption and lowering of postprandial hyperglycemia.

Because its mechanism of action is different, the effect of GLYSET to enhance glycemic control is additive to that of sulfonylureas when used in combination. In addition, GLYSET diminishes the insulinotropic and weight-increasing effects of sulfonylureas.

Miglitol has minor inhibitory activity against lactase and consequently, at the recommended doses, would not be expected to induce lactose intolerance.


 


Pharmacokinetics

Absorption

Absorption of miglitol is saturable at high doses: a dose of 25 mg is completely absorbed, whereas a dose of 100 mg is only 50% - 70% absorbed. For all doses, peak concentrations are reached in 2-3 hours. There is no evidence that systemic absorption of miglitol contributes to its therapeutic effect.

Distribution

The protein binding of miglitol is negligible ( < 4.0%). Miglitol has a volume of distribution of 0.18 L/kg, consistent with distribution primarily into the extracellular fluid.

Metabolism

Miglitol is not metabolized in man or in any animal species studied. No metabolites have been detected in plasma, urine, or feces, indicating a lack of either systemic or pre-systemic metabolism.

Excretion

Miglitol is eliminated by renal excretion as unchanged drug. Thus, following a 25-mg dose, over 95% of the dose is recovered in the urine within 24 hours. At higher doses, the cumulative recovery of drug from urine is somewhat lower due to the incomplete bioavailability. The elimination half-life of miglitol from plasma is approximately 2 hours.

Special Populations

Renal Impairment

Because miglitol is excreted primarily by the kidneys, accumulation of miglitol is expected in patients with renal impairment. Patients with creatinine clearance 60 mL/min. Dosage adjustment to correct the increased plasma concentrations is not feasible because miglitol acts locally. Little information is available on the safety of miglitol in patients with creatinine clearance < 25 mL/min.

Hepatic impairment

Miglitol pharmacokinetics were not altered in cirrhotic patients relative to healthy control subjects. Since miglitol is not metabolized, no influence of hepatic function on the kinetics of miglitol is expected.

Gender

No significant difference in the pharmacokinetics of miglitol was observed between elderly men and women when body weight was taken into account.

Race

Several pharmacokinetic studies were conducted in Japanese volunteers, with results similar to those observed in Caucasians. A study comparing the pharmacodynamic response to a single 50-mg dose in Black and Caucasian healthy volunteers indicated similar glucose and insulin responses in both populations.

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Clinical Studies

Clinical Experience in Non-Insulin-Dependent Diabetes Mellitus (NIDDM) Patients on Dietary Treatment Only

GLYSET Tablets were evaluated in two U.S. and three non-U.S. controlled, fixed-dose, monotherapy studies, in which 735 patients treated with GLYSET were evaluated for efficacy analyses (see Table 1).

In Study 1, a one-year study in which GLYSET was evaluated as monotherapy and also as combination therapy, there was a statistically significantly smaller increase in mean glycosylated hemoglobin (HbA1c) over time in the miglitol 50 mg 3 times daily monotherapy arm compared to placebo. Significant reductions in mean fasting and postprandial plasma glucose levels and in mean postprandial insulin levels were observed in patients treated with GLYSET compared with the placebo group.

In Study 2, a 14-week study, there was a significant decrease in HbA1c in patients receiving GLYSET 50 mg 3 times daily or 100 mg 3 times daily compared to placebo. In addition, there were significant reductions in postprandial plasma glucose and postprandial serum insulin levels compared to placebo.

Study 3 was a 6-month dose-ranging trial evaluating GLYSET at doses from 25 mg 3 times daily to 200 mg 3 times daily. GLYSET produced a greater reduction in HbA1c than placebo at all doses, although the effect was statistically significant only at the 100 mg 3 times daily and 200 mg 3 times daily doses. In addition, all doses of GLYSET produced significant reductions in postprandial plasma glucose and postprandial insulin levels compared to placebo.

Studies 4 and 5 were 6-month studies evaluating GLYSET at 50 and 100 mg 3 times daily, and 100 mg 3 times daily, respectively. As compared to placebo, GLYSET produced significant reductions in HbA1c, as well as a significant reduction in postprandial plasma glucose in both studies at the doses employed.

Table 1 Results of Monotherapy Study with Glyset

Study Treatment HbA1c (%) 1-hour Postprandial Glucose (mg/dL)
Mean Change from Baseline* Treatment Effect** Mean Change from Baseline Treatment Effect**
1 (U.S.) Placebo +0.71 --- +24 ---
GLYSET 50 mg t.i.d.*** +0.13 -0.58† -39 -63†
2 (U.S.) Placebo +0.47 --- +15 ---
GLYSET 50 mg t.i.d. -0.22 -0.69† -52 -67†
GLYSET 100 mg t.i.d. -0.28 -0.75† -59 -74†
3 (non-U.S.) Placebo +0.18 --- +2 ---
GLYSET 25 mg t.i.d. -0.08 -0.26 -33 -35†
GLYSET 50 mg t.i.d. -0.22 -0.40 -45 -47†
GLYSET 100 mg t.i.d. -0.63 -0.81† -62 -64†
GLYSET 200 mg t.i.d.c -0.84 -1.02† -85 -87†
4 (non-U.S.) Placebo +0.01 --- +8 ---
GLYSET 50 mg t.i.d. -0.35 -0.36† -20 -28†
GLYSET 100 mg t.i.d. -0.57 -0.58† -25 -33†
5 (non-U.S.) Placebo +0.32 --- +17 ---
GLYSET 100 mg t.i.d. -0.43 -0.75† -38 -55†
* Mean baseline ranged from 7.54 to 8.72% in these studies.
** The result of subtracting the placebo group average.
*** t.i.d. = 3 times daily
† p ≤ 0.05
c Although results for the 200 mg 3 times daily are presented for completeness, the maximum recommended dosage of GLYSET is 100 mg 3 times daily.

Clinical Experience in NIDDM Patients Receiving Sulfonylureas

GLYSET was studied as adjunctive therapy to a background of maximal or near-maximal sulfonylurea (SFU) treatment in three large, double-blind, randomized studies (two U.S. and one non-U.S.) in which 471 patients treated with GLYSET were evaluated for efficacy (see Table 2).

Study 6 included patients under treatment with maximal doses of SFU at entry. At the end of this 14-week study, the mean treatment effects on glycosylated hemoglobin (HbA1c) were -0.82% and -0.74% for patients receiving GLYSET 50 mg 3 times daily plus SFU, and GLYSET 100 mg 3 times daily plus SFU, respectively.

Study 7 was a one-year study in which GLYSET at 25, 50 or 100 mg 3 times daily was added to a maximal dose of glyburide (10 mg twice daily). At the end of this study, the mean treatment effects on HbA1c of GLYSET when added to maximum glyburide therapy were -0.30%, -0.62%, and -0.73% with the 25, 50 and 100 mg 3 times daily dosages of GLYSET, respectively.

In Study 8, the addition of GLYSET 100 mg 3 times daily to a background of treatment with glyburide produced an additional mean treatment effect on HbA1c of -0.66%.

Table 2: Results of Combination Therapy with GLYSET Plus Sulfonylurea (SFU)

Study Treatment HbA1c (%) 1-hour Postprandial Glucose (mg/dL)
Mean Change from Baseline* Treatment Effect** Mean Change from Baseline Treatment Effect**
6 (U.S.) Placebo + SFU +0.33 --- -1 ---
GLYSET 50 mg t.i.d.*** + SFU -0.49 -0.82† -69 -68†
GLYSET 100 mg t.i.d. + SFU -0.41 -0.74† -73 -72†
7 (U.S.) Placebo + SFU +1.01 --- 48 ---
GLYSET 25 mg t.i.d. + SFU +0.71 -0.30 -2 -50†
GLYSET 50 mg t.i.d. + SFU +0.39 -0.62† -13 -61†
GLYSET 100 mg t.i.d. + SFU +0.28 -0.73† -33 -81†
8 (non-U.S.) Placebo + SFU +0.16 --- +10 ---
GLYSET 100 mg t.i.d. + SFU -0.50 -0.66† -36 -46†
* Mean baseline ranged from 8.56 to 9.16% in these studies.
** The result of subtracting the placebo group average.
*** t.i.d. = 3 times daily
† p ≤ 0.05

Dose-Response

Results from controlled, fixed-dose studies of Glyset as monotherapy or as combination treatment with a sulfonylurea were combined to derive a pooled estimate of the difference from placebo in the mean change from baseline in glycosylated hemoglobin (HbA1c) and postprandial plasma glucose as shown in Figures 1 and 2:

Figure 1: HbA1c (%) Mean Change From Baseline: Treatment Effect Pooled Results from Controlled Fixed-Dose Studies in Tables 1 and 2

Miglitol HbA1c (%) Mean Change From Baseline

Figure 2: 1-Hour Postprandial Plasma Glucose Mean Change From Baseline: Treatment Effect Pooled Results from Controlled Fixed-Dose Studies in Tables 1 and 2

Miglitol Postprandial Plasma Glucose Mean Change From Baseline

Because of its mechanism of action, the primary pharmacologic effect of miglitol is manifested as a reduction in postprandial plasma glucose, as shown previously in all of the major clinical trials. GLYSET was statistically significantly different from placebo at all doses in each of the individual studies with respect to effect on mean one-hour postprandial plasma glucose, and there is a dose response from 25 to 100 mg 3 times daily for this efficacy parameter.


 


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Indications and Usage

Glyset Tablets, as monotherapy, are indicated as an adjunct to diet to improve glycemic control in patients with non-insulin-dependent diabetes mellitus (NIDDM) whose hyperglycemia cannot be managed with diet alone. Glyset may also be used in combination with a sulfonylurea when diet plus either Glyset or a sulfonylurea alone do not result in adequate glycemic control. The effect of Glyset to enhance glycemic control is additive to that of sulfonylureas when used in combination, presumably because its mechanism of action is different.

In initiating treatment for NIDDM, diet should be emphasized as the primary form of treatment. Caloric restriction and weight loss are essential in the obese diabetic patient. Proper dietary management alone may be effective in controlling blood glucose and symptoms of hyperglycemia. The importance of regular physical activity when appropriate should also be stressed. If this treatment program fails to result in adequate glycemic control, the use of Glyset should be considered. The use of Glyset must be viewed by both the physician and patient as a treatment in addition to diet and not as a substitute for diet or as a convenient mechanism for avoiding dietary restraint.

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Contraindications

GLYSET Tablets are contraindicated in patients with:

  • Diabetic ketoacidosis
  • Inflammatory bowel disease, colonic ulceration, or partial intestinal obstruction, and in patients predisposed to intestinal obstruction
  • Chronic intestinal diseases associated with marked disorders of digestion or absorption, or with conditions that may deteriorate as a result of increased gas formation in the intestine
  • Hypersensitivity to the drug or any of its components.

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Precautions

General

Hypoglycemia

Because of its mechanism of action, GLYSET when administered alone should not cause hypoglycemia in the fasted or postprandial state. Sulfonylurea agents may cause hypoglycemia. Because GLYSET Tablets given in combination with a sulfonylurea will cause a further lowering of blood glucose, it may increase the hypoglycemic potential of the sulfonylurea, although this was not observed in clinical trials. Oral glucose (dextrose), whose absorption is not delayed by GLYSET, should be used instead of sucrose (cane sugar) in the treatment of mild-to-moderate hypoglycemia. Sucrose, whose hydrolysis to glucose and fructose is inhibited by GLYSET, is unsuitable for the rapid correction of hypoglycemia. Severe hypoglycemia may require the use of either intravenous glucose infusion or glucagon injection.

Loss of Control of Blood Glucose

When diabetic patients are exposed to stress such as fever, trauma, infection, or surgery, a temporary loss of control of blood glucose may occur. At such times, temporary insulin therapy may be necessary.

Renal Impairment

Plasma concentrations of GLYSET in renally impaired volunteers were proportionally increased relative to the degree of renal dysfunction. Long-term clinical trials in diabetic patients with significant renal dysfunction (serum creatinine > 2.0 mg/dL) have not been conducted. Therefore, treatment of these patients with GLYSET is not recommended.

Information for Patients

The following information should be provided to patients:

  • Glyset should be taken orally three times a day at the start (with the first bite) of each main meal. It is important to continue to adhere to dietary instructions, a regular exercise program, and regular testing of urine and/or blood glucose.
  • Glyset itself does not cause hypoglycemia even when administered to patients in the fasted state. Sulfonylurea drugs and insulin, however, can lower blood sugar levels enough to cause symptoms or sometimes life-threatening hypoglycemia. Because Glyset given in combination with a sulfonylurea or insulin will cause a further lowering of blood sugar, it may increase the hypoglycemic potential of these agents. The risk of hypoglycemia, its symptoms and treatment, and conditions that predispose to its development should be well understood by patients and responsible family members. Because Glyset prevents the breakdown of table sugar, a source of glucose (dextrose, D-glucose) should be readily available to treat symptoms of low blood sugar when taking Glyset in combination with a sulfonylurea or insulin.
  • If side effects occur with Glyset, they usually develop during the first few weeks of therapy. They are most commonly mild-to-moderate dose-related gastrointestinal effects, such as flatulence, soft stools, diarrhea, or abdominal discomfort, and they generally diminish in frequency and intensity with time. Discontinuation of drug usually results in rapid resolution of these gastrointestinal symptoms.

Laboratory Tests

Therapeutic response to GLYSET may be monitored by periodic blood glucose tests. Measurement of glycosylated hemoglobin levels is recommended for the monitoring of long-term glycemic control.

In 12 healthy males, concomitantly administered antacid did not influence the pharmacokinetics of miglitol.

Drug Interactions

Several studies investigated the possible interaction between miglitol and glyburide. In six healthy volunteers given a single dose of 5-mg glyburide on a background of 6 days treatment with miglitol (50 mg 3 times daily for 4 days followed by 100 mg 3 times daily for 2 days) or placebo, the mean Cmax and AUC values for glyburide were 17% and 25% lower, respectively, when glyburide was given with miglitol. In a study in diabetic patients in which the effects of adding miglitol 100 mg 3 times daily × 7 days or placebo to a background regimen of 3.5 mg glyburide daily were investigated, the mean AUC value for glyburide was 18% lower in the group treated with miglitol, although this difference was not statistically significant. Further information on a potential interaction with glyburide was obtained from one of the large U.S. clinical trials (Study 7) in which patients were dosed with either miglitol or placebo on a background of glyburide 10 mg twice daily. At the 6-month and 1-year clinic visits, patients taking concomitant miglitol 100 mg 3 times daily exhibited mean Cmax values for glyburide that were 16% and 8% lower, respectively, compared to patients taking glyburide alone. However, these differences were not statistically significant. Thus, although there was a trend toward lower AUC and Cmax values for glyburide when co-administered with Glyset, no definitive statement regarding a potential interaction can be made based on the foregoing three studies.

The effect of miglitol (100 mg 3 times daily × 7 days) on the pharmacokinetics of a single 1000-mg dose of metformin was investigated in healthy volunteers. Mean AUC and Cmax values for metformin were 12% to 13% lower when the volunteers were given miglitol as compared with placebo, but this difference was not statistically significant.

In a healthy volunteer study, co-administration of either 50 mg or 100 mg miglitol 3 times daily together with digoxin reduced the average plasma concentrations of digoxin by 19% and 28%, respectively. However, in diabetic patients under treatment with digoxin, plasma digoxin concentrations were not altered by co-administration of miglitol 100 mg 3 times daily × 14 days.

Other healthy volunteer studies have demonstrated that miglitol may significantly reduce the bioavailability of ranitidine and propranolol by 60% and 40%, respectively. No effect of miglitol was observed on the pharmacokinetics or pharmacodynamics of either warfarin or nifedipine.

Intestinal adsorbents (e.g., charcoal) and digestive enzyme preparations containing carbohydrate-splitting enzymes (e.g., amylase, pancreatin) may reduce the effect of Glyset and should not be taken concomitantly.

In 12 healthy males, concomitantly administered antacid did not influence the pharmacokinetics of miglitol.

Carcinogenesis, Mutagenesis, and Impairment of Fertility

Miglitol was administered to mice by the dietary route at doses as high as approximately 500 mg/kg body weight (corresponding to greater than 5 times the exposure in humans based on AUC) for 21 months. In a two-year rat study, miglitol was administered in the diet at exposures comparable to the maximum human exposures based on AUC. There was no evidence of carcinogenicity resulting from dietary treatment with miglitol.

In vitro, miglitol was found to be nonmutagenic in the bacterial mutagenesis (Ames) assay and the eukaryotic forward mutation assay (CHO/HGPRT). Miglitol did not have any clastogenic effects in vivo in the mouse micronucleus test. There were no heritable mutations detected in dominant lethal assay.

A combined male and female fertility study conducted in Wistar rats treated orally with miglitol at dose levels of 300 mg/kg body weight (approximately 8 times the maximum human exposure based on body surface area) produced no untoward effect on reproductive performance or capability to reproduce. In addition, survival, growth, development, and fertility of the offspring were not compromised.

Pregnancy

Teratogenic Effects

Pregnancy Category B

The safety of GLYSET in pregnant women has not been established. Developmental toxicology studies have been performed in rats at doses of 50, 150 and 450 mg/kg, corresponding to levels of approximately 1.5, 4, and 12 times the maximum recommended human exposure based on body surface area. In rabbits, doses of 10, 45, and 200 mg/kg corresponding to levels of approximately 0.5, 3, and 10 times the human exposure were examined. These studies revealed no evidence of fetal malformations attributable to miglitol. Doses of miglitol up to 4 and 3 times the human dose (based on body surface area), for rats and rabbits, respectively, did not reveal evidence of impaired fertility or harm to the fetus. The highest doses tested in these studies, 450 mg/kg in the rat and 200 mg/kg in the rabbit promoted maternal and/or fetal toxicity. Fetotoxicity was indicated by a slight but significant reduction in fetal weight in the rat study and slight reduction in fetal weight, delayed ossification of the fetal skeleton and increase in the percentage of non-viable fetuses in the rabbit study. In the peri-postnatal study in rats, the NOAEL (No Observed Adverse Effect Level) was 100 mg/kg (corresponding to approximately four times the exposure to humans, based on body surface area). An increase in stillborn progeny was noted at the high dose (300 mg/kg) in the rat peri-postnatal study, but not at the high dose (450 mg/kg) in the delivery segment of the rat developmental toxicity study. Otherwise, there was no adverse effect on survival, growth, development, behavior, or fertility in either the rat developmental toxicity or peri-postnatal studies. There are, however, no adequate and well-controlled studies in pregnant women. Because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if clearly needed.

Nursing Mothers

Miglitol has been shown to be excreted in human milk to a very small degree. Total excretion into milk accounted for 0.02% of a 100-mg maternal dose. The estimated exposure to a nursing infant is approximately 0.4% of the maternal dose. Although the levels of miglitol reached in human milk are exceedingly low, it is recommended that GLYSET not be administered to a nursing woman.

Pediatric Use

Safety and effectiveness of GLYSET in pediatric patients have not been established.

Geriatric Use

Of the total number of subjects in clinical studies of GLYSET in the United States, patients valid for safety analyses included 24% over 65, and 3% over 75. No overall differences in safety and effectiveness were observed between these subjects and younger subjects. The pharmacokinetics of miglitol were studied in elderly and young males (n=8 per group). At the dosage of 100 mg 3 times daily for 3 days, no differences between the two groups were found.

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Adverse Reactions

Gastrointestinal

Gastrointestinal symptoms are the most common reactions to GLYSET Tablets. In U.S. placebo-controlled trials, the incidences of abdominal pain, diarrhea, and flatulence were 11.7%, 28.7%, and 41.5% respectively in 962 patients treated with GLYSET 25-100 mg 3 times daily, whereas the corresponding incidences were 4.7%, 10.0%, and 12.0% in 603 placebo-treated patients. The incidence of diarrhea and abdominal pain tended to diminish considerably with continued treatment.

Dermatologic

Skin rash was reported in 4.3% of patients treated with GLYSET compared to 2.4% of placebo-treated patients. Rashes were generally transient and most were assessed as unrelated to GLYSET by physician-investigators.

Abnormal Laboratory Findings

Low serum iron occurred more often in patients treated with GLYSET (9.2%) than in placebo-treated patients (4.2%) but did not persist in the majority of cases and was not associated with reductions in hemoglobin or changes in other hematologic indices.

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Overdosage

Unlike sulfonylureas or insulin, an overdose of GLYSET Tablets will not result in hypoglycemia. An overdose may result in transient increases in flatulence, diarrhea, and abdominal discomfort. Because of the lack of extra-intestinal effects seen with GLYSET, no serious systemic reactions are expected in the event of an overdose.

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Dosage and Administration

There is no fixed dosage regimen for the management of diabetes mellitus with GLYSET Tablets or any other pharmacologic agent. Dosage of GLYSET must be individualized on the basis of both effectiveness and tolerance while not exceeding the maximum recommended dosage of 100 mg 3 times daily. GLYSET should be taken three times daily at the start (with the first bite) of each main meal. GLYSET should be started at 25 mg, and the dosage gradually increased as described below, both to reduce gastrointestinal adverse effects and to permit identification of the minimum dose required for adequate glycemic control of the patient.

During treatment initiation and dose titration (see below), one-hour postprandial plasma glucose may be used to determine the therapeutic response to GLYSET and identify the minimum effective dose for the patient. Thereafter, glycosylated hemoglobin should be measured at intervals of approximately three months. The therapeutic goal should be to decrease both postprandial plasma glucose and glycosylated hemoglobin levels to normal or near normal by using the lowest effective dose of GLYSET, either as monotherapy or in combination with a sulfonylurea.

Initial Dosage

The recommended starting dosage of GLYSET is 25 mg, given orally three times daily at the start (with the first bite) of each main meal. However, some patients may benefit by starting at 25 mg once daily to minimize gastrointestinal adverse effects, and gradually increasing the frequency of administration to 3 times daily.

Maintenance Dosage

The usual maintenance dose of GLYSET is 50 mg 3 times daily, although some patients may benefit from increasing the dose to 100 mg 3 times daily. In order to allow adaptation to potential gastrointestinal adverse effects, it is recommended that GLYSET therapy be initiated at a dosage of 25 mg 3 times daily, the lowest effective dosage, and then gradually titrated upward to allow adaptation. After 4 - 8 weeks of the 25 mg 3 times daily regimen, the dosage should be increased to 50 mg 3 times daily for approximately three months, following which a glycosylated hemoglobin level should be measured to assess therapeutic response. If, at that time, the glycosylated hemoglobin level is not satisfactory, the dosage may be further increased to 100 mg 3 times daily, the maximum recommended dosage. Pooled data from controlled studies suggest a dose-response for both HbA1c and one-hour postprandial plasma glucose throughout the recommended dosage range. However, no single study has examined the effect on glycemic control of titrating patients' doses upwards within the same study. If no further reduction in postprandial glucose or glycosylated hemoglobin levels is observed with titration to 100 mg 3 times daily, consideration should be given to lowering the dose. Once an effective and tolerated dosage is established, it should be maintained.

Maximum Dosage

The maximum recommended dosage of GLYSET is 100 mg 3 times daily. In one clinical trial, 200 mg 3 times daily gave additional improved glycemic control but increased the incidence of the gastrointestinal symptoms described above.

Patients Receiving Sulfonylureas

Sulfonylurea agents may cause hypoglycemia. There was no increased incidence of hypoglycemia in patients who took GLYSET in combination with sulfonylurea agents compared to the incidence of hypoglycemia in patients receiving sulfonylureas alone in any clinical trial.

However, GLYSET given in combination with a sulfonylurea will cause a further lowering of blood glucose and may increase the risk of hypoglycemia due to the additive effects of the two agents. If hypoglycemia occurs, appropriate adjustments in the dosage of these agents should be made.

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How is Supplied

GLYSET Tablets are available as 25 mg, 50 mg, and 100 mg white, round, film-coated tablets. The tablets are debossed with the word "GLYSET" on one side and the strength on the other side, as indicated below.

Strength NDC Tablet Identification
Front Back
Bottles of 100:
25 mg 0009-5012-01 GLYSET 25
50 mg 0009-5013-01 GLYSET 50
100 mg 0009-5014-01 GLYSET 100

Store at 25°C (77°F); excursions permitted to 15°-30°C (59°-86°F) [see USP Controlled Room Temperature].

Rx only

Distributed by Pfizer

Manufactured by:

Bayer HealthCare AG
Leverkusen, Germany
Glyset is a registered trademark of Bayer HealthCare Pharmaceuticals Inc used under license .

LAB-0167-6.0

last updated 05/2008

Glyset, miglitol, patient information (in plain English)

Detailed Info on Signs, Symptoms, Causes, Treatments of Diabetes


The information in this monograph is not intended to cover all possible uses, directions, precautions, drug interactions or adverse effects. This information is generalized and is not intended as specific medical advice. If you have questions about the medicines you are taking or would like more information, check with your doctor, pharmacist, or nurse.

back to: Browse all Medications for Diabetes

APA Reference
Staff, H. (2008, May 29). Glyset for Treatment of Diabetes - Glyset Full Prescribing Information, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/diabetes/medications/glyset-full-prescribing-information

Last Updated: March 10, 2016

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APA Reference
(2008, May 17). Thursday, November 6, 2008, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/healthyplace/artical/Thursday%2C-November-6%2C-2008

Last Updated: January 14, 2014

Friday, May 16, 2008

Welcome to the HealthyPlace.com Community. I look forward to reading your journal entries.

Deborah

APA Reference
(2008, May 16). Friday, May 16, 2008, HealthyPlace. Retrieved on 2024, December 28 from https://www.healthyplace.com/healthyplace/artical/Friday%2C-May-16%2C-2008

Last Updated: January 14, 2014