HORMONES: PANCREATIC

Pramlintide is indicated for the following:

• Type 1 diabetes, as an adjunct treatment for 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 for 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

A boxed warning concerning the potential for insulin-induced hypoglycemia is included in the official prescribing information. Prescribers are encouraged to read the entire prescribing information, including this warning, before prescribing pramlintide.

Prescribing Information

Frequently Asked Questions: Pancreatic Hormones

Amylin

What is amylin, and where is it produced?
What are the physiologic effects and mechanisms of action of amylin?
What are the effects of amylin deficiency?
How can amylin concentrations be measured? Is there an amylin assay available?
What are the ranges for the fasting and postprandial human plasma amylin concentrations?
Is there amylin resistance? Does amylin contribute to insulin resistance?
How is amylin different from leptin?
How is amylin different from somatostatin?
Does amylin work with the enzyme system that acarbose and miglitol inhibit?
Does amylin cause amyloid deposits?
Does amylin cause Alzheimer's disease?
Where may information or training on amylin be obtained?
What is pramlintide?
How does pramlintide differ from amylin?
What is glucagon?
What is the function of glucagon?
How is glucagon affected by endogenous amylin and by exogenous pramlintide?
Can pramlintide suppress the inappropriate postprandial rise in glucagon secretion?
Can long-term suppression of postprandial glucagon secretion improve long-term glycemic control?
Why is glucagon also a pharmaceutical product?
How is glucagon for injection used?
How is glucagon supplied?
What are the side effects of glucagon?
What happens in case of overdose with glucagon?
What if glucagon does not resolve the hypoglycemic episode?
Does amylin inhibit the secretion of glucagon in response to hypoglycemia?
Is there an assay for glucagon?
References

 
What is amylin, and where is it produced?
 
Amylin is the 37–amino acid product of a gene located on chromosome 12.1 It is a naturally occurring neuroendocrine hormone that is colocalized and cosecreted in the same secretory vesicles with insulin from pancreatic β (beta) cells.2,3 Small amounts of amylin have also been detected in pancreatic α (alpha) and δ (delta) cells,4,5 the stomach,6,7 and various neurons of the nervous system. Amylin and insulin are cosecreted in response to carbohydrate (glucose) and protein-derived amino acids following a meal stimulus.8,9 Experimental studies have shown that amylin complements the effects of insulin in postprandial glucose regulation through several centrally mediated effects.10
 
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What are the physiologic effects and mechanisms of action of amylin?
 
Nearly 60 different effects of amylin have been identified in extensive in vitro and in vivo studies.10
Recent studies have identified at least 4 physiologic effects of amylin that complement insulin in regulating postprandial glucose homeostasis. These effects and their respective mechanisms of
action are as follows:

• Reduction of postprandial glucagon secretion and therefore the reduction of endogenous glucagon-stimulated hepatic glucose output.11 The mechanism by which amylin suppresses glucagon secretion has not been directly determined; however, possibilities include a central effect, a direct effect on the α cell, and a reduced rate of exposure to protein nutrients that stimulate glucagon secretion because of a reduced rate of gastric emptying. Results from preclinical studies indicate that this action is mediated centrally.
  
• Regulation of gastric emptying and therefore the rate of nutrient delivery (exogenous glucose)
  to the small intestine.12 Amylin-sensitive neurons in the area postrema, acting via a vagal pathway, are implicated in the regulation of gastric emptying. Results also support the presence of a regulatory feedback mechanism via glucose-sensitive amylinergic neurons present in the area postrema whereby hypoglycemia can override the regulation of gastric emptying by amylin.
  
• Reduction in food intake and therefore the reduction of exogenous glucose entering the circulation.13 As with the effect of amylin on gastric emptying, the effect on food intake appears
  to be mediated via amylin receptors located in the area postrema. However, this effect does not appear to involve vagal transmission. In one recent trial, patients with type 2 diabetes who were administered pramlintide had their nutrient intake reduced by 23% from baseline.14
  
• Reduction in body weight, which is at least partially due to a reduction in food intake

Amyloid deposits are a principal feature of Alzheimer's-disease pathology and a major factor in the disease process.24 The deposits are composed primarily of amyloid-β peptide amyloid deposits, a completely different protein from amylin.24

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Where may information or training on amylin be obtained?

 An educational Web site, www.amylin.org, has information on the amylin hormone. This site also includes an animated video with an overview of the physiology of amylin, slides, and further background educational materials. This Web site is sponsored by Amylin Pharmaceuticals, Inc.
 
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What is pramlintide?
 
Pramlintide is a synthetic analogue of human amylin recently approved for treatment of type 1 and
type 2 diabetes. Pramlintide is a 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)5,6,11 (Pro-h-amylin). It is the first member of a new class of therapeutic agents known as amylinomimetic agents, or amylin receptor agonists. Pramlintide was specifically engineered as a replacement for the naturally occurring neuroendocrine hormone amylin.25,26 Preclinical and clinical studies have documented various physiologic actions of pramlintide and its clinical effect as an adjunct to insulin therapy for diabetes.10

Pramlintide improves glucose control through prevention of the postprandial rise in plasma
glucagon27 and modulation of gastric emptying, both of which slow the rate of glucose appearance
into the circulation.28-30 

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How does pramlintide differ from amylin?
 
Pramlintide differs from human amylin in that 3 amino acid residues, 25Alanine, 28Serine, and
29Serine, have been replaced with prolines. Because of this replacement, pramlintide is a stable, soluble, nonaggregating, and nonadhesive peptide, whereas amylin is less stable in solution
and has the propensity to aggregate and adhere to surfaces.31

Figure 1. Control of blood glucose in healthy individuals

Figure 2. Possible mechanism of action of amylin in glucose homeostasis
(illustration adapted from Ludvik, et al)

To assess the regulation of glucagon secretion in type 2 disease, Fineman and coworkers36 compared postprandial glucagon and glucose levels during 5-hour intravenous infusions of either pramlintide or placebo in a single-blind, placebo-controlled crossover study of 24 patients with type 2 diabetes. AUCs for both postprandial plasma glucagon and glucose were significantly reduced during pramlintide infusions compared with placebo. These effects were equivalent in subgroup analyses of patients taking insulin or oral sulfonylureas.

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Can long-term suppression of postprandial glucagon secretion improve long-term
glycemic control?
 
Evidence indicates that suppression of postprandial glucagon may improve glycemic control.
Ratner and associates37 studied 538 insulin-treated patients with type 2 disease over a period of
52 months. Patients were randomized to receive 30, 75, or 150 mcg pramlintide or placebo 3 times daily at major meals. The results showed a mean reduction of glycosylated hemoglobin (A1C) of
0.9% and 1.0% in the groups receiving 75 and 150 mcg pramlintide, respectively; this reduction was significant compared with placebo. Because pramlintide functions by 2 routes—reduction of gastric emptying and downregulation of postprandial glucagon secretion—it is likely that the regulation of glucagon had some positive effect on long-term glycemia; however, the magnitude of the glucagon effect cannot be quantified separately from the gastric emptying effect.
 
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Why is glucagon also a pharmaceutical product?
 
Patients with diabetes who take insulin or oral insulin secretagogues, such as sulfonylureas, to control their blood glucose may, at times, encounter states wherein their blood glucose levels are extremely low (severe hypoglycemia) for any of several reasons, such as too much medication, taking medication without eating on schedule, or exercising after taking medication. In such a state, the patient may become unconscious and not able to swallow carbohydrates. The amount of glucagon within the body may not be enough to stimulate the release of enough glucose to supply the brain.38-41 For this reason, pharmaceutical companies manufacture glucagon for injection, usually in the form of a glucagon kit.
 
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How is glucagon for injection used?
 
In severe hypoglycemic episodes, glucagon from emergency kits may be injected intravenously, intramuscularly, or subcutaneously. Intramuscular and subcutaneous injections are generally
performed outside the hospital setting. For intramuscular and subcutaneous injections, glucagon reaches maximal plasma concentrations in approximately 15 and 20 minutes, respectively. Maximal glucose concentrations are attained within 30 minutes by either injection route. (It is important to
note that the patient will likely be unconscious during a severe hypoglycemic episode. The injection
will therefore be performed by someone other than the patient: preferably, a family member or friend who can recognize the symptoms of hypoglycemia and knows how to administer glucagon.) The
person performing the injection should lay the patient on his or her side in case of vomiting, an infrequent but potential side effect of the injection. Once the patient regains consciousness, usually within 15 minutes, glucose, in the form of food, should be provided, and the patient's doctor should
be notified.42
 
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How is glucagon supplied?
 
Glucagon is typically supplied as a dry powder in an emergency kit. A diluent solution is also
provided in the kit. The diluent is added to the glucagon and mixed. The resulting mixture is then injected immediately. Any unused portion of the mixed glucagon solution should be discarded
following resolution of the hypoglycemic episode.42
 
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What are the side effects of glucagon?
 
Adverse reactions are very rare but may include nausea, vomiting, and headache. Some people
may have an allergic reaction to animal-derived glucagon, but allergic reactions to glucagon produced by recombinant DNA techniques are extremely rare. Allergic reactions typically take the form of itching or development of a rash.42
 
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What happens in case of overdose with glucagon?
 
Overdose of glucagon is extremely rare. Because glucagon is rapidly metabolized and excreted, treatment of an overdose may be targeted to the symptoms (nausea, vomiting, diarrhea, and perhaps a transient increase in blood pressure). However, a local poison-control center should be contacted immediately by calling 1-800-222-1222. If difficulty in breathing or loss of consciousness occurs as a result of a glucagon injection, emergency assistance should be immediately sought.42
 
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What if glucagon does not resolve the hypoglycemic episode?
 
If the patient does not regain consciousness, an additional injection of glucagon may be performed,
but emergency aid should be sought because it may be necessary to administer intravenous glucose to the patient.42 Immediate attention may be very important, as continued severe hypoglycemia may cause neurologic damage.
 
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Does amylin inhibit the secretion of glucagon in response to hypoglycemia?
 
The suppressive effects of amylin on glucagon are lost in the presence of hypoglycemia. In a glycemic clamp study, Silvestre and associates43 showed that amylin did not reduce secretion of glucagon compared with placebo when blood glucose was reduced to 36 mg/dL (2 mmol/L).
 
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Is there an assay for glucagon?
 
Yes, a blood test can be performed.44 Plasma concentrations of glucagon in healthy subjects are generally in the range of 20 to 100 ng/L; however, values in patients with diabetes are generally much higher (approximately 1500 ng/L). In addition to its use in diabetes, the assay provides diagnostic information in glucagonoma; chronic renal failure; hyperlipoproteinemia; severe stress due to infections, trauma, burns, and surgery; familial hyperglucagonemia; cirrhosis; and various other hepatic and pancreatic disorders.
 
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