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Pegvisomant (Somavert) for Acromegaly

Pegvisomant (Somavert) inhibits the binding of growth hormone to its receptors resulting in the reduction of IGF-1 levels.
It is used to treat patients with acromegaly (excessive growth hormone production usually due to a pituitary adenoma) who respond poorly to surgery or radiation therapy, or when surgery and radiation therapy are inappropriate. The endocrine society recommends the use of pegvisomant postoperatively in patients with a persistent significant disease without mass effects. In mild disease, alternative agents may be preferred.

Pegvisomant dose in Adults

Pegvisomant dose in the treatment of Acromegaly:

An initial loading dose of 40 mg subQ
Maintenance dose:
- 10 mg once a day beginning the day after the initial loading dose.
The dose may be adjusted at 4 - 6 weeks intervals (based on IGF-1 levels) by increments of 5 mg.
The recommended dosing range is 10 - 30 mg/day.
The maximum dose is 30 mg/day.

Note: If the patient is not responding to the maximum dose (clinical or biochemical response based on IGF-1 levels), combination therapy should be considered. Combination therapy may include pegvisomant plus a somatostatin analog or pegvisomant plus a dopamine agonist.

Pegvisomant use in children:

It has not been studied in children

Pregnancy Risk Factor C

Pegvisomant should not be used during pregnancy. However, there are limited data.
Alternative therapies should be considered if the patient requires treatment for acromegaly, such as in cases where there is evidence of tumor growth or headaches from mass effects.
It is not advised to monitor IGF-1 levels during pregnancy.
Effective contraception should be recommended to women with reproductive potential, as it may restore fertility.
The Endocrine Society recommends that you stop taking octreotide at least two months before a planned pregnancy. You can also use short-acting octreotide.

Pegvisomant use during breastfeeding:

It is unknown if the drug will be excreted into breastmilk.
It is recommended that you use it with caution if you are breastfeeding.

Dose in kidney disease:

The manufacturer has not recommended any dose adjustment in patients with kidney disease.

Dose in liver disease:

At initiation of therapy:
- Patients with normal liver function test (LFT):
  - Adjustment in the dose is not necessary.
  - Liver function tests should be monitored monthly for the first 6 months, quarterly for the next 6 months, and then every 6 monthly.
- Patients with baseline LFT less than 3 times the ULN elevated:
  - Adjustment in the dose is not necessary.
  - Liver function tests should be monitored monthly for one year and then every 6 monthly.
- Patients with baseline LFTs greater than 3 times the ULN:
  - Treatment should not be initiated.
  - Gallstones or a history of gallstones should be ruled out especially in patients with a prior history of octreotide analog therapy.
  - LFTs should be monitored closely in these patients.
With ongoing therapy:
- Patients with LFTs 3 - 5 the ULN but without clinical features of hepatitis, hepatic injury or raised bilirubin:
  - Treatment may be continued, however, LFTs should be monitored weekly.
  - Alternative causes of hepatic injury should be ruled out.
- LFTs more than 5 times the ULN or transaminase more than 3 times the ULN associated with any increase in total bilirubin (with or without clinical features of hepatitis):
  - Treatment should be discontinued promptly.
  - Treatment may be reinitiated after the LFTs return to baseline, however, frequent monitoring is required.
- Features of hepatic injury or hepatitis:
  - Treatment should be permanently discontinued and immediate hepatic workup and treatment should be initiated.

Common Side Effects of Pegvisomant Include:

Central Nervous System:
- Pain
Gastrointestinal:
- Diarrhea
- Nausea
Hepatic:
- Abnormal Hepatic Function Tests
Immunologic:
- Antibody Development
Infection:
- Infection
Local:
- Injection Site Reaction
Respiratory:
- Flu-Like Symptoms

Pegvisomant side effects (less common):

Cardiovascular:
- Chest Pain
- Hypertension
- Peripheral Edema
Central Nervous System:
- Dizziness
- Paresthesia
Endocrine & Metabolic:
- Lipohypertrophy
Neuromuscular & Skeletal:
- Back Pain
Respiratory:
- Sinusitis
Miscellaneous:
- Accidental Injury

Contraindication to Pegvisomant Include:

You may have severe allergic reactions to any ingredient of the formulation or the drug.

Warnings and precautions

Hepatic effects
- It can cause liver function tests to be elevated.
- Despite the use of ALT, there have been cases of transient but marked elevations (up to 15x the normal upper limit) of ALT.
- Patients with liver disease or pre-existing conditions should not use the therapy. Liver function should be closely monitored during treatment.
- Patients with hepatic toxicities should stop taking the medication.
Hypersensitivity
- It has been associated with allergic reactions such as anaphylaxis and laryngeal swelling, angioedemas, rash, urticaria and pruritis.
- It is possible to consider re-initiating treatment with caution.
Lipohypertrophy
- After repeated administration to a single site, lipohypertrophy can occur.
- To reduce the risk of lipohypertrophy, rotate the injection site daily.
Diabetes:
- Diabetes patients should be closely monitored as this may lead to an increase in glucose tolerance.
- It is possible that you will need to adjust your anti-diabetic medications.

Pegvisomant: Drug Interaction

Risk Factor C (Monitor therapy)
Blood Glucose Lowering Agents	Pegvisomant may enhance the hypoglycemic effect of Blood Glucose Lowering Agents.
Opioid Agonists	May diminish the therapeutic effect of Pegvisomant.
Pegloticase	May diminish the therapeutic effect of PEGylated Drug Products.
Pegvaliase	PEGylated Drug Products may enhance the adverse/toxic effect of Pegvaliase. Specifically, the risk of anaphylaxis or hypersensitivity reactions may be increased.
Somatostatin Analogs	May enhance the adverse/toxic effect of Pegvisomant. Specifically, this combination may increase the risk for significant elevations of liver enzymes.
Risk Factor X (Avoid combination)
Macimorelin	Growth Hormone Products may diminish the diagnostic effect of Macimorelin.

Monitor:

Assess the GH-secreting tumor size every 6 to 12 months after the initiation of therapy and then yearly (based on tumor size) with MRI.
Monitor blood sugars in diabetic patients.
Monitor serum IGF-1 levels 4 - 6 weeks after the start of therapy and after the dose is changed and every 6 months once normalized.
Monitor liver injury or dysfunction.

Monitor:

LFTs (Liver function tests) as:
At the initiation of therapy:
- Patients with normal liver function test (LFT):
  - Adjustment in the dose is not necessary.
  - Liver function tests should be monitored monthly for the first 6 months, quarterly for the next 6 months, and then every 6 monthly.
- Patients with baseline LFT less than 3 times the ULN elevated:
  - Adjustment in the dose is not necessary.
  - Liver function tests should be monitored monthly for one year and then every 6 monthly.
- Patients with baseline LFTs greater than 3 times the ULN:
  - Treatment should not be initiated.
  - Gallstones or a history of gallstones should be ruled out especially in patients with a prior history of octreotide analog therapy.
  - LFTs should be monitored closely in these patients.

With ongoing therapy:
- Patients with LFTs 3 - 5 the ULN but without clinical features of hepatitis, hepatic injury or raised bilirubin:
  - Treatment may be continued, however, LFTs should be monitored weekly.
  - Alternative causes of hepatic injury should be ruled out.
- LFTs more than 5 times the ULN or transaminase more than 3 times the ULN associated with any increase in total bilirubin (with or without clinical features of hepatitis):
  - Treatment should be discontinued promptly.
  - Treatment may be reinitiated after the LFTs return to baseline, however, frequent monitoring is required.
- Features of hepatic injury or hepatitis:
  - Treatment should be permanently discontinued and immediate hepatic workup and treatment should be initiated.

How to administer Pegvisomant?

Its route of administration is subcutaneous only.
The injection site should be rotated daily to avoid lipo-hypertrophy.
Patients who require two injections, both should be injected at different sites.
The injection may be administered in the upper arm, upper thigh, buttocks, or abdomen.
Avoid rubbing the injection site. It should not be injected into a broken, infected, or bruised skin.
Injection into a lump or a rash should also be avoided.
The first injection should be administered under the supervision of a healthcare provider.

Pegvisomant mechanism of action:

It acts as an antagonist of growth hormone receptors.
Pegvisomant binding inhibits growth hormone binding to its receptors, resulting in a decrease in insulin-like growth factor (IGF-1) release.
This blocks excessive growth hormone production in the body, as seen in patients with growth hormone secreting pituitary tumors.

Nearly half(57%) of the drug is absorbedAfter subQ administration.

Distribution: 7 L

Half-life elimination: abiut 60 to 138 hours (~2.5 to 6 days)

Time to reach peak serum concentration: 33 - 77 hours

Excretion: Urine (<1%)