d with long-term use. peliosis hepatis and hepatic adenoma may be silent until complicated by acute, potentially life-threatening intraabdominal hemorrhage. the physician therefore should be alert to this possibility. attempts should be made to determine the lowest dose that will provide adequate protection. if the drug was begun at a time of exacerbation of hereditary angioneurotic edema due to trauma, stress or other cause, periodic attempts to decrease or withdraw therapy should be considered. danazol has been associated with several cases of benign intracranial hypertension also known as pseudotumor cerebri. early signs and symptoms of benign intracranial hypertension include papilledema, headache, nausea and vomiting, and visual disturbances. patients with these symptoms should be screened for papilledema and, if present, the patients should be advised to discontinue danazol immediately and be referred to a neurologist for further diagnosis and care. a temporary alteration of lipoproteins in the form of decreased high density lipoproteins and possibly increased low density lipoproteins has been reported during danazol therapy. these alterations may be marked, and prescribers should consider the potential impact on the risk of atherosclerosis and coronary artery disease in accordance with the potential benefit of the therapy to the patient. patients should be watched closely for signs of androgenic effects some of which may not be reversible even when drug administration is stopped.

ents for continuous treatment of hereditary angioedema with danazol capsules should be individualized on the basis of the clinical response of the patient. it is recommended that the patient be started on 200 mg, two or three times a day. after a favorable initial response is obtained in terms of prevention of episodes of edematous attacks, the proper continuing dosage should be determined by decreasing the dosage by 50% or less at intervals of one to three months or longer if frequency of attacks prior to treatment dictates. if an attack occurs, the daily dosage may be increased by up to 200 mg. during the dose adjusting phase, close monitoring of the patient's response is indicated, particularly if the patient has a history of airway involvement.

e, viscosity, sperm count, and motility may occur in patients receiving long-term therapy. hepatic dysfunction, as evidenced by reversible elevated serum enzymes and/or jaundice, has been reported in patients receiving a daily dosage of danazol capsules of 400 mg or more. it is recommended that patients receiving danazol capsules be monitored for hepatic dysfunction by laboratory tests and clinical observation. serious hepatic toxicity including cholestatic jaundice, peliosis hepatis, hepatic adenoma, hepatocellular injury, hepatocellular jaundice and hepatic failure have been reported (see warnings and precautions ). abnormalities in laboratory tests may occur during therapy with danazol capsules including cpk, glucose tolerance, glucagon, thyroid binding globulin, sex hormone binding globulin, other plasma proteins, lipids and lipoproteins. the following reactions have been reported, a causal relationship to the administration of danazol capsules has neither been confirmed nor refuted; allergic: urticaria, pruritus and rarely, nasal congestion; cns effects: headache, nervousness and emotional lability, dizziness and fainting, depression, fatigue, sleep disorders, tremor, paresthesias, weakness, visual disturbances, and rarely, benign intracranial hypertension, anxiety, changes in appetite, chills, and rarely convulsions, guillain-barre syndrome; gastrointestinal: gastroenteritis, nausea, vomiting, constipation, and rarely, pancreatitis and splenic peliosis; musculoskeletal: muscle cramps or spasms, or pains, joint pain, joint lockup, joint swelling, pain in back, neck, or extremities, and rarely, carpal tunnel syndrome which may be secondary to fluid retention; genitourinary: hematuria, prolonged posttherapy amenorrhea; hematologic: an increase in red cell and platelet count. reversible erythrocytosis, leukocytosis or polycythemia may be provoked. eosinophilia, leukopenia and thrombocytopenia have also been noted. skin: rashes (maculopapular, vesicular, papular, purpuric, petechial), and rarely, sun sensitivity, stevens-johnson syndrome and erythema multiforme; other: increased insulin requirements in diabetic patients, change in libido, myocardial infarction, palpitation, tachycardia, elevation in blood pressure, interstitial pneumonitis, and rarely, cataracts, bleeding gums, fever, pelvic pain, nipple discharge. malignant liver tumors have been reported in rare instances, after long-term use.

al tissue so that it becomes inactive and atrophic. complete resolution of endometrial lesions occurs in the majority of cases. changes in vaginal cytology and cervical mucus reflect the suppressive effect of danazol on the pituitary-ovarian axis. changes in the menstrual pattern may occur. generally, the pituitary-suppressive action of danazol is reversible. ovulation and cyclic bleeding usually return within 60 to 90 days when therapy with danazol is discontinued. in the treatment of hereditary angioedema, danazol at effective doses prevents attacks of the disease characterized by episodic edema of the abdominal viscera, extremities, face, and airway which may be disabling and, if the airway is involved, fatal. in addition, danazol corrects partially or completely the primary biochemical abnormality of hereditary angioedema by increasing the levels of the deficient c1 esterase inhibitor (c1ei). as a result of this action the serum levels of the c4 component of the complement system are also increased. pharmacokinetics absorption: after oral administration of a 400 mg dose to healthy male volunteers, peak plasma concentrations of danazol are reached between 2 and 8 hours, with a median t max value of 4 hours. steady state conditions are observed following 6 days of twice daily dosing of danazol capsules. the pharmacokinetic parameters for danazol capsules after administering a 400 mg oral dose to healthy males are summarized in the following table: parameters mean ± sd (n=15) c max (ng/ml) 69.6 ± 29.9 t max (h) 2.47 ± 1.62 auc 0-∞ (ng*h/ml) 601 ± 181 t 1/2 (h) 9.70 ± 3.29 total body clearance (l/h) 727 ± 221 the pharmacokinetic parameters for danazol capsules after oral administration of 100, 200 and 400 mg single doses to healthy female volunteers are summarized in the following table: dose (mg) mean c max ± sd (ng/ml) mean t max (h) mean auc 0-∞ ± sd (ng*h/ml) fasting fed fasting fed fasting fed 100 45.9 ± 23.9 113.8 ± 46.0 1-8 2-6 484 ± 263 741 ± 265 200 63.8 ± 27.7 159 ± 57.3 1-6 2-4 681 ± 363 1252 ± 307 400 60.4 ± 30.0 253.7 ± 105.5 1-6 2-4 754 ± 443 1851 ± 605 dose proportionality: bioavailability studies indicate that blood levels do not increase proportionally with increases in the administered dose. single dose administration of danazol capsules in healthy female volunteers found that a 4-fold increase in dose produced only a 1.6 and 2.5-fold increase in auc and a 1.3 and 2.2-fold increase in c max in the fasted and fed state, respectively. a similar degree of non-dose proportionality was observed at steady state. food effect: single dose administration of 100 mg and 200 mg capsules of danazol to female volunteers showed that both the extent of availability and the maximum plasma concentration increased by 3 to 4 fold, respectively, following a meal (> 30 grams of fat), when compared to the fasted state. further, food also delayed mean time to peak concentration of danazol by about 30 minutes. even after multiple dosing under less extreme food/fasting conditions, there remained approximately a 2 to 2.5 fold difference in bioavailability between the fed and fasted states. distribution: danazol is lipophilic and can partition into cell membranes, indicating the likelihood of distribution into deep tissue compartments. metabolism and excretion: danazol appears to be metabolized and the metabolites are eliminated by renal and fecal pathways. the two primary metabolites excreted in the urine are 2-hydroxymethyl danazol and ethisterone. at least ten different products were identified in feces. the reported elimination half-life of danazol is variable across studies. the mean half-life of danazol in healthy males is 9.7 h. after 6 months of 200 mg three times a day dosing in endometriosis patients, the half-life of danazol was reported as 23.7 hours.

63 741 ± 265 200 63.8 ± 27.7 159 ± 57.3 1-6 2-4 681 ± 363 1252 ± 307 400 60.4 ± 30.0 253.7 ± 105.5 1-6 2-4 754 ± 443 1851 ± 605 dose proportionality: bioavailability studies indicate that blood levels do not increase proportionally with increases in the administered dose. single dose administration of danazol capsules in healthy female volunteers found that a 4-fold increase in dose produced only a 1.6 and 2.5-fold increase in auc and a 1.3 and 2.2-fold increase in c max in the fasted and fed state, respectively. a similar degree of non-dose proportionality was observed at steady state. food effect: single dose administration of 100 mg and 200 mg capsules of danazol to female volunteers showed that both the extent of availability and the maximum plasma concentration increased by 3 to 4 fold, respectively, following a meal (> 30 grams of fat), when compared to the fasted state. further, food also delayed mean time to peak concentration of danazol by about 30 minutes. even after multiple dosing under less extreme food/fasting conditions, there remained approximately a 2 to 2.5 fold difference in bioavailability between the fed and fasted states. distribution: danazol is lipophilic and can partition into cell membranes, indicating the likelihood of distribution into deep tissue compartments. metabolism and excretion: danazol appears to be metabolized and the metabolites are eliminated by renal and fecal pathways. the two primary metabolites excreted in the urine are 2-hydroxymethyl danazol and ethisterone. at least ten different products were identified in feces. the reported elimination half-life of danazol is variable across studies. the mean half-life of danazol in healthy males is 9.7 h. after 6 months of 200 mg three times a day dosing in endometriosis patients, the half-life of danazol was reported as 23.7 hours.