in addition, clinical cases of adrenal insufficiency have been observed in patients receiving or being withdrawn from chronic megestrol acetate therapy in the stressed and non-stressed state. furthermore, adrenocorticotropin (acth) stimulation testing has revealed the frequent occurrence of asymptomatic pituitary-adrenal suppression in patients treated with chronic megestrol acetate therapy. therefore, the possibility of adrenal insufficiency should be considered in any patient receiving or being withdrawn from chronic megestrol acetate therapy who presents with symptoms and/or signs suggestive of hypoadrenalism (e.g., hypotension, nausea, vomiting, dizziness, or weakness) in either the stressed or non-stressed state. laboratory evaluation for adrenal insufficiency and consideration of replacement or stress doses of a rapidly acting glucocorticoid are strongly recommended in such patients. failure to recognize inhibition of the hypothalamic-pituitary-adrenal axis may result in death. finally, in patients who are receiving or being withdrawn from chronic megestrol acetate therapy, consideration should be given to the use of empiric therapy with stress doses of a rapidly acting glucocorticoid in conditions of stress or serious intercurrent illness (e.g., surgery, infection).

2 3 0 1 urinary frequency 0 0 1 2 5 2 1 adverse events which occurred in 1 to 3% of all patients enrolled in the two clinical efficacy trials with at least one follow-up visit during the first 12 weeks of the study are listed below by body system. adverse events occurring less than 1% are not included. there were no significant differences between incidence of these events in patients treated with megestrol acetate and patients treated with placebo. body as a whole - abdominal pain, chest pain, infection, moniliasis and sarcoma cardiovascular system - cardiomyopathy and palpitation digestive system - constipation, dry mouth, hepatomegaly, increased salivation and oral moniliasis hemic and lymphatic system - leukopenia metabolic and nutritional - ldh increased, edema and peripheral edema nervous system - paresthesia, confusion, convulsion, depression, neuropathy, hypesthesia and abnormal thinking respiratory system - dyspnea, cough, pharyngitis and lung disorder skin and appendages - alopecia, herpes, pruritus, vesiculobullous rash, sweating and skin disorder special senses - amblyopia urogenital system - albuminuria, urinary incontinence, urinary tract infection and gynecomastia postmarketing - postmarketing reports associated with megestrol acetate oral suspension included thromboembolic phenomena including thrombophlebitis and pulmonary embolism and glucose intolerance (see warnings and precautions ).

ight, diet and liver function. the major route of drug elimination in humans is urine. when radiolabeled megestrol acetate was administered to humans in doses of 4 to 90 mg, the urinary excretion within 10 days ranged from 56.5 to 78.4% (mean 66.4%) and fecal excretion ranged from 7.7 to 30.3% (mean 19.8%). the total recovered radioactivity varied between 83.1 and 94.7% (mean 86.2%). megestrol acetate metabolites which were identified in urine constituted 5 to 8% of the dose administered. respiratory excretion as labeled carbon dioxide and fat storage may have accounted for at least part of the radioactivity not found in urine and feces. plasma steady state pharmacokinetics of megestrol acetate were evaluated in 10 adult, cachectic male patients with acquired immunodeficiency syndrome (aids) and an involuntary weight loss greater than 10% of baseline. patients received single oral doses of 800 mg/day of megestrol acetate oral suspension for 21 days. plasma concentration data obtained on day 21 were evaluated for up to 48 hours past the last dose. mean (±1sd) peak plasma concentration (c max ) of megestrol acetate was 753 (±539) ng/ml. mean area under the concentration time-curve (auc) was 10476 (±7788) ng × hr/ml. median t max value was five hours. seven of 10 patients gained weight in three weeks. additionally, 24 adult, asymptomatic hiv seropositive male subjects were dosed once daily with 750 mg of megestrol acetate oral suspension. the treatment was administered for 14 days. mean c max and auc values were 490 (±238) ng/ml and 6779 (±3048) hr × ng/ml, respectively. the median t max value was three hours. the mean c min value was 202 (±101) ng/ml. the mean % of fluctuation value was 107 (±40). the effect of food on the bioavailability of megestrol acetate oral suspension has not been evaluated.

currently available. impairment of fertility perinatal/postnatal (segment iii) toxicity studies were performed in rats at doses (0.05 to 12.5 mg/kg) less than that indicated for humans (13.3 mg/kg); in these low dose studies, the reproductive capability of male offspring of megestrol acetate-treated females was impaired. similar results were obtained in dogs. pregnant rats treated with megestrol acetate showed a reduction in fetal weight and number of live births, and feminization of male fetuses. no toxicity data are currently available on male reproduction (spermatogenesis).

mg ma group by 1.9 pounds and decreased in the placebo group by 1.6 pounds. mean weight changes at 4, 8 and 12 weeks for patients evaluable for efficacy in the two clinical trials are shown graphically. changes in body composition during the 12 study weeks as measured by bioelectrical impedance analysis showed increases in non-water body weight in the ma-treated groups (see clinical studies table ). in addition, edema developed or worsened in only 3 patients. greater percentages of ma-treated patients in the 800 mg group (89%), the 400 mg group (68%) and the 100 mg group (72%), than in the placebo group (50%), showed an improvement in appetite at last evaluation during the 12 study weeks. a statistically significant difference was observed between the 800 mg ma-treated group and the placebo group in the change in caloric intake from baseline to time of maximum weight change. patients were asked to assess weight change, appetite, appearance, and overall perception of well-being in a 9 question survey. at maximum weight change only the 800 mg ma-treated group gave responses that were statistically significantly more favorable to all questions when compared to the placebo-treated group. a dose response was noted in the survey with positive responses correlating with higher dose for all questions. the second trial was a multicenter, randomized, double-blind, placebo-controlled study comparing megestrol acetate 800 mg/day versus placebo in aids patients with anorexia/cachexia and significant weight loss. of the 100 patients entered on study, 65 met all inclusion/exclusion criteria, had at least two additional post baseline weight measurements over a 12 week period or had one post baseline weight measurement but dropped out for therapeutic failure. patients in the 800 mg ma-treated group had a statistically significantly larger increase in mean maximum weight change than patients in the placebo group. from baseline to study week 12, mean weight increased by 11.2 pounds in the ma-treated group and decreased 2.1 pounds in the placebo group. changes in body composition as measured by bioelectrical impedance analysis showed increases in non-water weight in the ma-treated group (see clinical studies table ). no edema was reported in the ma-treated group. a greater percentage of ma-treated patients (67%) than placebo-treated patients (38%) showed an improvement in appetite at last evaluation during the 12 study weeks; this difference was statistically significant. there were no statistically significant differences between treatment groups in mean caloric change or in daily caloric intake at time to maximum weight change. in the same 9 question survey referenced in the first trial, patients' assessments of weight change, appetite, appearance, and overall perception of well-being showed increases in mean scores in ma-treated patients as compared to the placebo group. in both trials, patients tolerated the drug well and no statistically significant differences were seen between the treatment groups with regard to laboratory abnormalities, new opportunistic infections, lymphocyte counts, t 4 counts, t 8 counts, or skin reactivity tests (see adverse reactions ). megestrol acetate oral suspension clinical efficacy trials trial 1 study accrual dates 11/88 to 12/90 trial 2 study accrual dates 5/89 to 4/91 megestrol acetate, mg/day 0 100 400 800 0 800 entered patients 38 82 75 75 48 52 evaluable patients 28 61 53 53 29 36 mean change in weight (lb.) baseline to 12 weeks 0.0 2.9 9.3 10.7 -2.1 11.2 % patients ≥5 pound gain at last evaluation in 12 weeks 21 44 57 64 28 47 mean changes in body composition based on bioelectrical impedance analysis determinations at last evaluation in 12 weeks. fat body mass (lb.) 0.0 2.2 2.9 5.5 1.5 5.7 lean body mass (lb.) -1.7 -0.3 1.5 2.5 -1.6 -0.6 water (liters) -1.3 -0.3 0.0 0.0 -0.1 -0.1 % patients with improved appetite: at time of maximum weight change 50 72 72 93 48 69 at last evaluation in 12 weeks 50 72 68 89 38 67 mean change in daily caloric intake: baseline to time of maximum weight change -107 326 308 646 30 464 the following figures are the results of mean weight changes for patients evaluable for efficacy in trials 1 and 2. trial 1 trial 2