About The Drug Pergolide Mesylate aka Permax
Find Pergolide Mesylate side effects, uses, warnings, interactions and indications. Pergolide Mesylate is also known as Permax.
Pergolide Mesylate
About Pergolide Mesylate aka Permax |
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What's The Definition Of The Medical Condition Pergolide Mesylate?Clinical Pharmacology CLINICAL PHARMACOLOGY Pharmacodynamic Information Pergolide mesylate is a potent dopamine receptor agonist.
Pergolide is 10 to 1,000 times more potent than bromocriptine on a milligram per milligram basis in various in vitro and in vivo test systems.
Pergolide mesylate inhibits the secretion of prolactin in humans; it causes a transient rise in serum concentrations of growth hormone and a decrease in serum concentrations of luteinizing hormone.
In Parkinson†s disease, pergolide mesylate is believed to exert its therapeutic effect by directly stimulating postsynaptic dopamine receptors in the nigrostriatal system.
Pharmacokinetic Information (Absorption, Distribution, Metabolism, and Elimination) Information on oral systemic bioavailability of pergolide mesylate is unavailable because of the lack of a sufficiently sensitive assay to detect the drug after the administration of a single dose.
However, following oral administration of 14C radiolabeled pergolide mesylate, approximately 55% of the administered radioactivity can be recovered from the urine and 5% from expired CO2, suggesting that a significant fraction is absorbed.
Nothing can be concluded about the extent of presystemic clearance, if any.
Data on postabsorption distribution of pergolide are unavailable.
At least 10 metabolites have been detected, including N-despropyl-pergolide, pergolide sulfoxide, and pergolide sulfone.
Perolide sulfoxide and pergolide sulfone are dopamine agonists in animals.
The other detected metabolites have not been identified and it is not known whether any other metabolites are active pharmacologically.
The major route of excretion is the kidney.
Pergolide is approximately 90% bound to plasma proteins.
This extent of protein binding may be important to consider when pergolide mesylate is coadministered with other drugs known to affect protein binding.
Drug Description DESCRIPTION Permax (pergolide mesylate) is an ergot derivative dopamine receptor agonist at both D1 and D2 receptor sites.
Pergolide mesylate is chemically designated as 8B-[(Methylthio)methyl]-6-propylergoline monomethanesulfonate.
The formula weight of the base is 314.5; 1 mg of base corresponds to 3.18 µmol.
Permax (pergolide mesylate) is provided for oral administration in tablets containing 0.05 mg (0.159 µmol), 0.25 mg (0.795 µmol), or 1 mg (3.18 µmol) pergolide as the base.
The tablets also contain croscarmel lose sodium, iron oxide, lactose, magnesium stearate, and povidone.
The 0.05-mg tablet also contains methionine, and the 0.25mg tablet also contains FD&C Blue No.2.
Indications & Dosage INDICATIONS Permax (pergolide mesylate) is indicated as adjunctive treatment to levodopa/carbidopa in the management of the signs and symptoms of Parkinson†s disease.
Evidence to support the efficacy of pergolide mesylate as an antiparkinsonian adjunct was obtained in a multicenter study enrolling 376 patients with mild to moderate Parkinson†s disease who were intolerant to l-dopa/carbidopa as manifested by moderate to severe dyskinesia and/or on-off phenomena.
On average, the patients evaluated had been on l-dopa/carbidopa for 3.9 years (range, 2 days to 16.8 years).
The administration of pergolide mesylate permitted a 5% to 30% reduction in the daily dose of l/dopa.
On average, these patients treated with pergolide mesylate maintained an equivalent or better clinical status than they exhibited at baseline.
DOSAGE AND ADMINISTRATION Administration of Permax (pergolide mesylate) should be initiated with a daily dosage of 0.05 mg for the first 2 days.
The dosage should then be gradually increased by 0.1 or 0.15 mg/day every third day over the next 12 days of therapy.
The dosage may then be increased by 0.25 mg/day every third day until an optimal therapeutic dosage is achieved.
Permax (pergolide mesylate) is usually administered in divided doses 3 times per day.
During dosage titration, the dosage of concurrent l-dopa/carbidopa may be cautiously decreased.
In clinical-studies, the mean therapeutic daily dosage of Permax (pergolide mesylate) was 3 mg/day.
The average concurrent daily dosage of l-dopa/carbidopa (expressed as l-dopa) was approximately 650 mg/day.
The efficacy of Permax (pergolide mesylate) at doses above 5 mg/day has not been systematically evaluated.
HOW SUPPLIED Tablets (scored): 0.05 mg, ivory, debossed with A615, (UC5336)-(RxPak* of 30) NDC 59075-615-30 0.25 mg, green, debossed with A625, (UC5337)-(RxPak of 100) NDC 59075-625-10 1 mg, pink, debossed with A630, (UC5338)--(RxPak of 100) NDC 59075-630-10 *All RxPaks (prescription packages, Lilly) have safety closures.
Store at controlled room temperature, 59 to 86° F (15 to 30° C ).
CAUTION-Federal (USA) law prohibits dispensing without prescription.
Updated Apr 08, 2003
Medication Guide PATIENT INFORMATION Patients and their families should be informed of the common adverse consequences of the use of pergolide mesylate (see ADVERSE REACTIONS) and the risk of hypotension (see WARNINGS ).
Patients should be advised to notify their physician if they become pregnant or intend to become pregnant during therapy.
Patients should be advised to notify their physician if they are breast feeding an infant.
Overdosage & Contraindications OVERDOSE There is no clinical experience with massive overdosage.
The largest overdose involved a young hospitalized adult patient who was not being treated with pergolide mesylate but who intentionally took 60 mg of the drug.
He experienced vomiting, hypotension, and agitation.
Another patient receiving a daily dosage of 7 mg of pergolide mesylate unintentionally took 19 mg/day for 3 days, after which his vital signs were normal but he experienced severe hallucinations.
Within 36 hours of resumption of the prescribed dosage level, the hallucinations stopped.
One patient unintentionally took 14 mg/day for 23 days instead of her prescribed 1.4 mg/day dosage.
She experienced severe involuntary movements and tingling in her arms and legs.
Another patient who inadvertently received 7 mg instead of the prescribed 0.7 mg experienced palpitations, hypotension, and ventricular extrasystoles.
The highest total daily dose (prescribed for several patients with refractory Parkinson†s disease) has exceeded 30 mg.
Symptoms Animal studies indicate that the manifestations of over-dosage in man might include nausea, vomiting, convulsions, decreased blood pressure, and CNS stimulation.
The oral median lethal doses in mice and rats were 54 and 15 mg/kg respectively.
Treatment To obtain up-to-date information about the treatment of overdose, a good resource is your certified Regional Poison Control Center.
Telephone numbers of certified poison control centers are listed in the Physicians Desk Reference (PDR).
In managing overdosage, consider the possibility of multiple drug overdoses, interaction among drugs, and unusual drug kinetics in your patient.
Management of overdosage may require supportive measures to maintain arterial blood pressure.
Cardiac function should be monitored; an antiarrhythmic agent may be necessary.
If signs of CNS stimulation are present, a phenothiazine or other butvronhenone neuroleptic agent may be indicated; the efficacy of such drugs in reversing the effects of overdose has not been assessed.
Protect the patient†s airway and support ventilation and perfusion.
Meticulously monitor and maintain, within acceptable limits, the patient†s vital signs, blood gases, serum electrolytes, etc..
Absorption of drugs from the gastrointestinal tract may be decreased by giving activated charcoal, which, in many cases, is more effective than emesis or lavage; consider charcoal instead of or in addition to gastric emptying.
Repeated doses of charcoal over time may hasten elimination of some drugs that have been absorbed.
Safeguard the patient†s airway when employing gastric emptying or charcoal.
There is no experience with dialysis or hemoperfusion, and these procedures are unlikely to be of benefit.
CONTRAINDICATIONS Pergolide mesylate is contraindicated in patients who are hypersensitive to this drug or other ergot derivatives.
Side Effects & Drug Interactions SIDE EFFECTS Commonly Observed In premarketing clinical trials, the most commonly observed adverse events associated with use of pergolide mesylate which were not seen at an equivalent incidence among placebo-treated patients were: nervous system complaints, including dyskinesia, hallucinations, somnolence, insomnia; digestive complaints, including nausea, constipation, diarrhea, dyspepsia; and respiratory system complaints, including rhinitis.
Associated With Discontinuation of Treatment Twenty-seven percent (27%) of approximately 1,200 patients receiving pergolide mesylate for treatment of Parkinson†s disease in premarketing clinical trials in the US and Canada discontinued treatment due to adverse events.
The events most commonly causing discontinuation were related to the nervous system (15.5%), primarily hallucinations (7.8%) and confusion (1.8%).
Fatalities-See WARNINGS.
Incidence in Controlled Clinical Trials The table that follows enumerates adverse events that occurred at a frequency of 1% or more among patients taking pergolide mesylate who participated in the premarketing controlled clinical trials comparing pergolide mesylate with placebo.
In a double-blind, controlled study of 6 month†s duration, patients with Parkinson†s disease were continued on l-dopa/carbidopa and were randomly assigned to receive either pergolide mesylate or placebo as additional therapy.
The prescriber should be aware that these figures cannot be used to predict the incidence of side effects in the course of usual medical practice where patient characteristics and other factors differ from those which prevailed in the clinical trials.
Similarly, the cited frequencies cannot be compared with figures obtained from other clinical investigations involving different treatments, uses, and investigators.
The cited figures, however, do provide the prescribing physician with some basis for estimating the relative contribution of drug and nondrug factors to the side-effect incidence rate in the population studied.
Incidence of Treatment-Emergent Adverse Experiences in the Placebo-Controlled Clinical Trial Percentage of Patients Reporting Events Body System/Adverse Event* Pergolide Mesylate Placebo N= 189 N= 187 Body as a Whole Pain 7.0 2.1 Abdominal pain 5.8 2.1 Injury, accident 5.8 7.0 Headache 5.3 6.4 Asthenia 4.2 4.8 Chest pain 3.7 2.1 Flu syndrome 3.2 2.1 Neck pain 2.7 1.6 Back pain 1.6 2.1 Surgical procedure 1.6 < 1 Chills 1.1 0 Face edema 1.1 0 Infection 1.1 0 Cardiovascular Postural hypotension 9.0 7.0 Vasodilatation 3.2 < 1 Palpitation 2.1 < 1 Hypotension 2.1 < 1 Syncope 2.1 1.1 Hypertension 1.6 1.1 Arrhythmia 1.1 < 1 Myocardial infarction 1.1 < 1 Digestive Nausea 24.3 12.8 Constipation 10.6 5.9 Diarrhea 6.4 2.7 Dyspepsia 6.4 2.1 Anorexia 4.8 2.7 Dry mouth 3.7 < 1 Vomiting 2.7 1.6 Hemic and Lymphatic Anemia 1.1 < 1 Metabolic and Nutritional Peripheral edema 7.4 4.3 Edema 1.6 0 Weight gain 1.6 0 Musculoskeletal Arthralgia 1.6 2.1 Bursitis 1.6 < 1 Myalgia 1.1 < 1 Twitching 1.1 0 Nervous System Dyskinesia 62.4 24.6 Dizziness 19.1 13.9 Hallucinations 13.8 3.2 Dystonia 11.6 8.0 Confusion 11.1 9.6 Somnolence 10.1 3.7 Insomnia 7.9 3.2 Anxiety 6.4 4.3 Tremor 4.2 7.5 Depression 3.2 5.4 Abnormal dreams 2.7 4.3 Personality disorder 2.1 < 1 Psychosis 2.1 0 Abnormal gait 1.6 1.6 Akathisia 1.6 0 Extrapyramidal syndrome 1.6 1.1 Incoordination 1.6 < 1 Paresthesia 1.6 3.2 Akinesia 1.1 1.1 Hypertonia 1.1 0 Neuralgia 1.1 < 1 Speech disorder 1.1 1.6 Respiratory System Rhinitis 12.2 5.4 Dyspnea 4.8 1.1 Epistaxis 1.6 < 1 Hiccup 1.1 0 Skin and Appendages Rash 3.2 2.1 Sweating .
2.1 2.7 Special Senses Abnormal vision 5.8 5.4 Diplopia 2.1 0 Taste perversion 1.6 0 Eye disorder 1.1 0 Urogenital Svstem Urinary frequency 2.7 6.4 Urinary tract infection 2.7 3.7 Hematuria 1.1 < 1 *Events reported by at least 1% of patients receiving pergolide mesylate are included.
Events Observed During the Premarketing Evaluation of Permax (pergolide mesylate) This section reports event frequencies evaluated as of October 1988 for adverse events occurring in a group of approximately 1,800 patients who took multiple doses of pergolide mesylate.
The conditions and duration of exposure to pergolide mesylate varied greatly, involving well-controlled studies as well as experience in open and uncontrolled clinical settings.
In the absence of appropriate controls in some of the studies, a causal relationship between these events and treatment with pergolide mesylate cannot be determined.
The following enumeration by organ system describes events in terms of their relative frequency of reporting in the data base.
Events of major clinical importance are also described in the Warnings and Precautions sections.
The following definitions of frequency are used: frequent adverse events are defined as those occurring in at least 1/100 patients; infre-quent adverse events are those occurring in 1/100 to 1/1,000 patients; rare events are those occurring in fewer than l/1,000 patients.
Body as a Whole - Frequent: headache asthenia, accidental injury, pain, abdominal pain, chest pain, back pain, flu syndrome, neck pain, fever; Infrequent: facial edema, chills, enlarged abdomen, malaise, neoplasm, hernia, pelvic pain, sepsis, cellulitis, moniliasis, abscess, jaw pain, hypothermia; Rare: acute abdominal syndrome, LE syndrome Cardiovascular System - Frequent: postural hypotension, syncope, hypertension, palpitations, vasodilatations, congestive heart failure; Infrequent: myocardial infarction, tachycardia, heart arrest, abnormal electrocardiogram, angina pectoris, thrombophlebitis, bradycardia, ventricular extrasystoles, cerebrovascular accident, ventricular tachycardia, cerebral ischemia, atrial fibrillation, varicose vein, pulmonary embolus, AV block, shock; Rare: vasculitis, pulmonary hypertension, pericarditis, migraine, heart block, cerebral hemorrhage Digestive System - Frequent: nausea, vomiting, dyspepsia, diarrhea, constipation, dry mouth, dysphagia; Infrequent: flatulence, abnormal liver function tests, increased appetite, salivary gland enlargement, thirst, gastroenteritis, gastritis, periodontal abscess, intestinal obstruction, nausea and vomiting, gingivitis, esophagitis, cholelithiasis, tooth caries, hepatitis, stomach ulcer, melena, hepatomegaly, hematemesis, eructation; Rare: sialadenitis, peptic ulcer, pancreatitis, jaundice, glossitis, fecal incontinence, duodenitis, colitis, cholecystitis, aphthous stomatitis, esophageal ulcer Endocrine System - Infrequent: hypothyroidism, adenoma, diabetes mellitus, ADH inappropriate; Rare: endocrine disorder, thyroid adenoma Hemic and Lymphatic System - Frequent: anemia; Infrequent: leukopenia, lymphadenopathy, leukocytosis, thrombocytopenia, petechia, megaloblastic anemia, cyanosis; Rare: purpura, lymphocytosis, eosinophilia, thrombocythemia, acute lymphoplastic leukemia, polycythemia, splenomegaly Metabolic and Nutritional System - Frequent: peripheral edema, weight loss, weight gain; Infrequent: dehydration, hypokalemia, hypoglycemia, iron deficiency anemia, hyperglycemia, gout, hyper-cholesteremia; Rare: electrolyte imbalance, cachexia, acidosis, hyperuricemia Musculoskeletal System - Frequent: twitching, myalgia, arthralgia; Infrequent: bone pain, tenosynovitis, myositis, bone sarcoma, arthritis; Rare: osteoporosis, muscle atrophy, osteomyelitis Nervous System - Frequent: dyskinesia, dizziness, hallucinations, confusion, somnolence, insomnia, dystonia, paresthesia, depression, anxiety, tremor, akinesia, extrapyramidal syndrome, abnormal gait, abnormal dreams, incoordination, psychosis, personality disorder, nervousness, choreoathetosis, amnesia, paranoid reaction, abnormal thinking; Infrequent: akathisia, neuropathy, neuralgia, hypertonia, delusions, convulsion, libido increased, euphoria, emotional lability, libido decreased, vertigo, myoclonus, coma, apathy, paralysis, neurosis, hyperkinesia, ataxia, acute brain syndrome, torticollis, meningitis, manic reaction, hypokinesia, hostility, agitation, hypotonia; Rare: stupor, neuritis, intracranial hypertension, hemiplegia, facial paralysis, brain edema, myelitis, hallucinations and confusion after abrupt discontinuation Respiratory System - Frequent: rhinitis, dyspnea, pneumonia, pharyngitis, cough increased; Infrequent: epistaxis, hiccup, sinusitis, bronchitis, voice alteration, hemoptysis, asthma, lung edema, pleural effusion, laryngitis, emphysema, apnea, hyperventilation; Rare: pneumothorax, lung fibrosis, larynx edema, hypoxia, hypoventilation, hemothorax, carcinoma of lung Skin and Appendages System - Frequent: sweating, rash; Infrequent: skin discoloration, pruritus, acne, skin ulcer, alopecia, dry skin, skin carcinoma, seborrhea, hirsutism, herpes simplex, eczema, fungal dermatitis, herpes zoster; Rare: vesiculobullous rash, subcutaneous nodule, skin nodule, skin benign neoplasm, lichenoid dermatitis Special Senses System - Frequent: abnormal vision, diplopia; Infrequent: otitis media, conjunctivitis, tinnitus, deafness, taste perversion, ear pain, eye pain, glaucoma, eye hemorrhage, photophobia, visual field defect; Rare: blindness, cataract, retinal detachment, retinal vascular disorder Urogenital System - Frequent: urinary tract infection, urinary frequency, urinary incontinence, hematuria, dysmenorrhea; Infrequent: dysuria, breast pain, menorrhagia, impotence, cystitis, urinary retention, abortion, vaginal hemorrhage, vaginitis, priapism, kidney calculus, fibrocystic breast, lactation, uterine hemorrhage, urolithiasis, salpingitis, pyuria, metrorrhagia, menopause, kidney failure, breast carcinoma, cervical carcinoma; Rare: amenorrhea, bladder carcinoma, breast engorgement, epididymitis, hypogonadism, leukorrhea, nephrosis, pyelonephritis, urethral pain, uricaciduria, withdrawal bleeding.
Postintroduction Reports - Voluntary reports of adverse events temporally associated with pergolide that have been received since market Introduction and which may have no causal relationship with the drug, include the following: neuroleptic malignant syndrome.
DRUG INTERACTIONS Dopamine antagonists, such as the neuroleptics (phenothiazines, butyrophenones, thioxanthines ) or metoclopramide, ordinarily should not be administered concurrently with Permax (pergolide mesylate) (a dopamine agonist); these agents may diminish the effectiveness of Permax.
Because pergolide mesylate is approximately 90% bound to plasma proteins, caution should be exercised if pergolide mesylate is coadministered with other drugs known to affect protein binding.
Warnings & Precautions WARNINGS Symptomatic Hypotension In clinical trials, approximately 10 % of patients taking pergolide mesylate with l-dopa versus 7% taking placebo with l-dopa experienced symptomatic orthostatic and/or sustained hypotension, especially during initial treatment.
With gradual dosage titration, tolerance to the hypotension usually develops.
It is therefore important to warn patients of the risk, to begin therapy with low doses, and to increase the dosage in carefully adjusted increments over a period of 3 to 4 weeks (see DOSAGE AND ADMININSTRATION).
Hallucinosis In controlled trials, pergolide mesylate with l-dopa caused hallucinosis in about 14% of patients as opposed to 3% taking placebo with l-dopa.
This was of sufficient severity to cause discontinuation of treatment in about 3% of those enrolled; tolerance to this untoward effect was not observed.
Fatalities In the placebo-controlled trial, 2 of 187 patients treated with placebo died as compared with 1 of 189 patients treated with pergolide mesylate.
Of the 2,299 patients treated with pergolide mesylate in premarketing studies evaluated as of October 1988, 143 died while on the drug or shortly after discontinuing it.
Because the patient population under evaluation was elderly, ill, and at high risk for death, it seems unlikely that pergolide mesylate played any role in these deaths, but the possibility that pergolide shortens survival of patients cannot be excluded with absolute certainty.
In particular, a case-by-case review of the clinical course of the patients who died failed to disclose any unique set of signs, symptoms, or laboratory results that would suggest that treatment with pergolide caused their deaths.
Sixty-eight percent (68%) of the patients who died were 65 years of age or older.
No death (other than a suicide) occurred within the first month of treatment; most of the patients who died had been on pergolide for years.
A relative frequency of the causes of death by organ system are: Pulmonary failure/Pneumonia, 35%; Cardiovascular, 30%; Cancer, 11%; Unknown, 8.4%; Infection, 3.5%; Extrapyramidal syndrome, 3.5%; Stroke, 2.1%; Dysphagia, 2.1%; Injury, 1 .4 %; Suicide, 1.4%; Dehydration, 0.7%; Glomerulonephritis, 0.7%.
Serious Inflammation and Fibrosis There have been rare reports of pleuritis, pleural effusion, cardiac valvulopathy involving one or more valves, pleural fibrosis, pericarditis, pericardial effusion or retroperitoneal fibrosis in patients taking pergolide.
In some cases, symptoms or manifestations of cardiac valvulopathy improved after discontinuation of pergolide.
Some patients had experienced similar events while taking the ergot derivative bromocriptine.
Pergolide should be used with caution in patients with a history of these conditions, particularly those patients who experienced the events while taking ergot derivatives.
Patients with a history of such events should be carefully monitored clinically and with appropriate radiographic and laboratory studies while taking pergolide.
PRECAUTIONS General Caution should be exercised when administering pergolide mesylate to patients prone to cardiac dysrhythmias.
In a study comparing pergolide mesylate and placebo, patients taking pergolide mesylate were found to have signifiscantly more episodes premature contractions (PACs) and sinus tachycardia.
The use of pergolide mesylate in patients on l-dopa may cause and/or exacerbate preexisting states of confusion and hallucinations (see WARNINGS) and preexisting dyskinesia.
Also, the abrupt discontinuation of pergolide mesylate in patients receiving it chronically as an adjunct to l-dopa may precipitate the onset of hallucinations and confusion; these may occur within a span of several days.
Discontinuation of pergolide should be undertaken gradually whenever possible, even if the patient is to remain on l-dopa.
A symptom complex resembling the neuroleptic malignant syndrome (NMS) (characterized by elevated temperature, muscular rigidity, altered consciousness, and autonomic instability), with no other obvious etiology has been reported in association with rapid dose reduction, with drawal of, or changes in antiparkinsonian therapy, including pergolide.
Information for Patients Patients and their families should be informed of the common adverse consequences of the use of pergolide mesylate (see ADVERSE REACTIONS) and the risk of hypotension (see WARNINGS ).
Patients should be advised to notify their physician if they become pregnant or intend to become pregnant during therapy.
Patients should be advised to notify their physician if they are breast feeding an infant.
Laboratory Tests No specific laboratory tests are deemed essential for the management of patients on Permax (pergolide mesylate) .
Periodic routine evaluation of all patients, however, is appropriate.
Drug Interactions Dopamine antagonists, such as the neuroleptics (phenothiazines, butyrophenones, thioxanthines ) or metoclopramide, ordinarily should not be administered concurrently with Permax (pergolide mesylate) (a dopamine agonist); these agents may diminish the effectiveness of Permax.
Because pergolide mesylate is approximately 90% bound to plasma proteins, caution should be exercised if pergolide mesylate is coadministered with other drugs known to affect protein binding.
Carcinogenesis, Mutagenesis, and Impairment of Fertility A 2-year carcinogenicity study was conducted in mice using dietary levels of pergolide mesylate equivalent to oral doses of 0.6, 3.7, and 36.4 mg/kg/day in males and 0.6, 4.4, and 40.8 mg/kg/day in females.
A 2-year study in rats was conducted using dietary levels equivalent to oral doses of 0.04, 0.18, and 0.88 mg/kg/day in males and 0.05, 0.28, and 1.42 mg/kg/day in females.
The highest doses tested in the mice and rats were approximately 340 and 12 times the maximum human oral dose administered in controlled clinical trials (6 mg/day equivalent to 0.12 mg/kg/day).
A low incidence of uterine neoplasms occurred in both rats and mice.
Endometrial adenomas and carcinomas were observed in rats.
Endometrial sarcomas were observed in mice.
The occurrence of these neoplasms is probably attributable to the high estrogen/progesterone ratio that would occur in rodents as a result of the prolactin-inhibiting action of pergolide mesylate.
The endocrine mechanisms believed to be involved in the rodents are not present in humans.
However, even though there is no known correlation between uterine malignancies occurring in pergolide-treated rodents and human risk, there are no human data to substantiate this conclusion.
Pergolide mesylate was evaluated for mutagenic potential in a battery of tests that included an Ames bacterial mutation assay, a DNA repair assay in cultured rat hepatocytes, an in vitro mammalian cell-point- mutation assay in cultured L5178Y cells, and a determination of chromosome alteration in bone marrow cells of Chinese hamsters.
A weak mutagenic response was noted in the mammalian cell-point-mutation assay only after metabolic activation with rat liver microsomes.
No mutagenic effects were obtained in the 2 other in vitro assays and in the in vivo assay.
The relevance of these findings in humans is unknown.
A fertility study in male and female mice showed that fertility was maintained at 0.6 and 1.7 mg/kg/day but decreased at 5.6 mg/kg/day.
Prolactin has been reported to be involved in stimulating and maintaining progesterone levels required for implantation in mice and therefore, the impaired fertility at the high dose may have occurred because of decressed prolactin levels.
Usage in Pregnancy Pregnancy Category B: Reproduction studies were conducted in mice at doses of 5, 16, and 45 mg/kg/day and in rabbits at doses of 2, 6, and 16 mg/kg/day.
The highest doses tested in mice and rabbits were 375 and 133 times the 6 mg /day maximum human dose administered in controlled clinical trials.
In these studies, there was no evidence of harm to the fetus due to pergolide mesylate.
There are, however, no adequate and well-controlled studies in pregnant women.
Among women who received pergolide mesylate for endocrine disorders in premarketing studies, there were 33 pregnancies that resulted in healthy babies and 6 pregnancies that resulted in congenital abnormalities (3 major, 3 minor); a causal relationship has not been established.
Because human data are limited and because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if clearly needed.
Nursing Mothers It is not known whether this drug is excreted in human milk.
The pharmacologic action of pergolide mesylate suggests that it may interfere with lactation.
Because many drugs are excreted in human milk and because of the potential for serious adverse reactions to pergolide mesylate in nursing infants, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.
Pediatric Use Safety and effectiveness in pediatric patients have not been established.
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