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phosphate allergies |
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phosphate allergies DESCRIPTION Zafirlukast is a synthetic, selective peptide leukotriene receptor antagonist(LTRA), with the chemical name 4-(5-cyclopentyloxy-carbonylamino-1-methyl-indol-3-ylmethyl)-3-methoxy-N-o-tolylsulfonylbenzamide phosphate allergies. The molecular weight of zafirlukast is 575.7 and the structural formula is:
Zafirlukast, a fine white to pale yellow amorphous powder, is practically insolublein water phosphate allergies. It is slightly soluble in methanol and freely soluble in tetrahydrofuran,dimethylsulfoxide, and acetone phosphate allergies. ACCOLATE is supplied as 10 and 20 mg tablets for oral administration phosphate allergies. Inactive Ingredients: Film-coated tablets containing croscarmellose sodium,lactose, magnesium stearate, microcrystalline cellulose, povidone, hypromellose,and titanium dioxide phosphate allergies.
In vitro studies demonstrated that zafirlukast antagonized the contractileactivity of three leukotrienes (LTC 4 , LTD 4 and LTE 4 ) in conducting airwaysmooth muscle from laboratory animals and humans phosphate allergies. Zafirlukast prevented intradermalLTD 4 -induced increases in cutaneous vascular permeability and inhibited inhaledLTD 4 -induced influx of eosinophils into animal lungs phosphate allergies. Inhalational challengestudies in sensitized sheep showed that zafirlukast suppressed the airway responsesto antigen; this included both the early- and late-phase response and the nonspecifichyperresponsiveness phosphate allergies. In humans, zafirlukast inhibited bronchoconstriction caused by several kindsof inhalational challenges phosphate allergies. Pretreatment with single oral doses of zafirlukastinhibited the bronchoconstriction caused by sulfur dioxide and cold air in patientswith asthma phosphate allergies. Pretreatment with single doses of zafirlukast attenuated the early-and late-phase reaction caused by inhalation of various antigens such as grass,cat dander, ragweed, and mixed antigens in patients with asthma phosphate allergies. Zafirlukastalso attenuated the increase in bronchial hyperresponsiveness to inhaled histaminethat followed inhaled allergen challenge phosphate allergies. Clinical Pharmacokinetics and Bioavailability: Distribution Metabolism Excretion In the pivotal bioequivalence study, the mean terminal half-life of zafirlukastis approximately 10 hours in both normal adult subjects and patients with asthma phosphate allergies. In other studies, the mean plasma half-life of zafirlukast ranged from approximately8 to 16 hours in both normal subjects and patients with asthma phosphate allergies. The pharmacokineticsof zafirlukast are approximately linear over the range from 5 mg to 80 mg phosphate allergies. Steady-stateplasma concentrations of zafirlukast are proportional to the dose and predictablefrom single-dose pharmacokinetic data phosphate allergies. Accumulation of zafirlukast in the plasmafollowing twice-daily dosing is approximately 45% phosphate allergies. The pharmacokinetic parameters of zafirlukast 20 mg administered as a singledose to 36 male volunteers are shown with the table below phosphate allergies. Mean (% Coefficient of Variation) pharmacokinetic
Race: No differences in the pharmacokinetics of zafirlukast due to race havebeen observed phosphate allergies. Elderly: The apparent oral clearance of zafirlukast decreases with age phosphate allergies. Inpatients above 65 years of age, there is an approximately 2-3 fold greater Cmax and AUC compared to young adult patients phosphate allergies. Children: Following administration of a single 20 mg dose of zafirlukast to20 boys and girls between 7 and 11 years of age, and in a second study, to 29boys and girls between 5 and 6 years of age, the following pharmacokinetic parameterswere obtained: Parameter Children age
Zafirlukast disposition was unchanged after multiple dosing (20 mg twice daily)in children and the degree of accumulation in plasma was similar to that observedin adults phosphate allergies. Hepatic Insufficiency: In a study of patients with hepatic impairment (biopsy-provencirrhosis), there was a reduced clearance of zafirlukast resulting in a 50-60%greater C max and AUC compared to normal subjects phosphate allergies. Renal Insufficiency: Based on a cross-study comparison, there are no apparentdifferences in the pharmacokinetics of zafirlukast between renally-impairedpatients and normal subjects phosphate allergies. Drug-Drug Interactions
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| pphosphate allergies phhosphate allergies phoosphate allergies phossphate allergies phospphate allergies phosphhate allergies phosphaate allergies phosphatte allergies phosphatee allergies phosphate allergies phosphate aallergies phosphate alllergies phosphate alllergies phosphate alleergies phosphate allerrgies phosphate allerggies phosphate allergiies phosphate allergiees phosphate allergiess hosphate allergies posphate allergies phsphate allergies phophate allergies phoshate allergies phospate allergies phosphte allergies phosphae allergies phosphat allergies phosphateallergies phosphate llergies phosphate alergies phosphate alergies phosphate allrgies phosphate allegies phosphate alleries phosphate allerges phosphate allergis phosphate allergie p hosphate allergies ph osphate allergies pho sphate allergies phos phate allergies phosp hate allergies phosph ate allergies phospha te allergies phosphat e allergies phosphate allergies phosphate allergies phosphate a llergies phosphate al lergies phosphate all ergies phosphate alle rgies phosphate aller gies phosphate allerg ies phosphate allergi es phosphate allergie s phosphate allergies hposphate allergies pohsphate allergies phsophate allergies phopshate allergies phoshpate allergies phospahte allergies phosphtae allergies phosphaet allergies phosphat eallergies phosphatea llergies phosphate lalergies phosphate allergies phosphate alelrgies phosphate allregies phosphate allegries phosphate alleriges phosphate allergeis phosphate allergise aphosphate allergies thephosphate allergies phosphate allergies | |||
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Copyright 2005 D-S LTD. |