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Ketoconazole Foods

KETOCONAZOLE This drug is given with food to minimize gastrointestinal irritation. Tablets may be crushed. Ketoconazole is absorbed best in an acid environment. Do not administer antacids, anticholinergics, or histamine blockers until at least 2 hours after ketoconazole is given. [Pg.135]

As a consequence of its high lipophilicity and low aqueous solubility, gastric acidity is also required for itraconazole absorption (Haria et al., 1996). It is best absorbed when administered with food, although there is considerable interpatient variabihty. The oral bioavailability or itraconazole from a 100-mg solution dose was 55%. Like ketoconazole, its bioavailability and half-life are dose-dependent, indicating saturable metabolism. Once absorbed, itraconazole is highly plasma protein bound (99.8%) and widely distributed (10.7 L/kg). Although itraconazole is widely metabolized, it does produce an active metabolite by hydroxylation of the triazolone side-chain. [Pg.74]

Nausea, vomiting, and anorexia occur commonly with ketoconazole, especially when high doses are prescribed. Epigastric distress can be reduced by taking ketoconazole with food. Pruritis and/or allergic dermatitis occurs in 10% of patients. Liver enzyme elevations during therapy are not unusual and are usually reversible. Severe ketoconazole-associated hepatitis is rare. [Pg.600]

Although specific drug or food interactions with mifepristone have not been studied, on the basis of this drug s metabolism by CYP3A4, it is possible that ketoconazole, itraconazole, erythromycin, and grapefruit juice may inhibit its metabolism (increasing serum levels of mifepristone). Furthermore, rifampin, dexamethasone, St. John s wort, and certain anticonvulsants (e.g., phenytoin, phenobarbital, and carbamazepine) may induce mifepristone metabolism (lowering serum levels of mifepristone)... [Pg.255]

Secondary> hyperparathyroidism 30 mg PO daily Parathyroid carcinoma 30 mg PO bid titrate q2—4wk based on Ca PTH levels swallow whole take w/ food Caution [C, /—] w/ Szs Disp Tabs SE N/V/D, myalgia, dizziness, 4- Ca2+ Interactions T Effects W/ CYP3A4 inhibitors such as ketoconazole, itraconazole, erythromycin T effects OF drugs metabolized at CYP2D6 such as TCA, thioridazine, flecainide, vinblastine EMS Monitor ECG for signs of hypocalcemia (T QT interval) OD May cause severe hypocalcemia calcium salts can be given... [Pg.112]

Pharmacokinetics Itraconazole is well-absorbed orally and food increases its bioavailability. It is extensively bound to plasma proteins and distributes well throughout most tissues, including bone, sputum and adipose tissues. However, therapeutic concentrations are not attained in the CSF. Like ketoconazole it is extensively metabolized in the liver but does not inhibit androgen synthesis. Little of the parent drug appears in the urine and thus doses do not have to be reduced in renal failure. [Pg.353]

AZOLES ANTACIDS i plasma concentration of itraconazole and ketoconazole, with risk of therapeutic failure Itraconazole absorption in capsule form requires an acidic gastric environment and thus absorption would l Separate administration of agents that i gastric acidity by 1-2 hours. However, absorption of itraconazole liquid solution does not require an acidic environment and could be used instead it does not need to be given with food. Fluconazole absorption is not pH dependent, and this is a suitable alternative... [Pg.564]

Ketoconazole is water-soluble at a pH of below 3. Its oral absorption is influenced by the acidity of the stomach contents, and the concomitant administration of histamine H2 receptor antagonists, proton pump inhibitors, antacids, or food affects its absorption. A high carbohydrate meal ingested with ketoconazole reduces total drug absorption, while a high lipid meal increases it. Erratic absorption is particularly apparent in patients with AIDS. Peak serum concentrations are seen within 2-3 hours. The half-life is about 8 hours. CSF penetration is less than 10% (1). Ketoconazole is extensively metabolized in the liver and excreted in the bile in an inactive form less than 1% of the active drug is excreted in the urine. Clearance is not significantly altered by renal dialysis (1). [Pg.1969]

Food and Drng Administration. Ketoconazole labeling revised. FDA Drng Bnll 1984 14(2) 17-18. [Pg.1975]

See other pages where Ketoconazole Foods is mentioned: [Pg.122]    [Pg.505]    [Pg.76]    [Pg.99]    [Pg.112]    [Pg.132]    [Pg.163]    [Pg.176]    [Pg.233]    [Pg.234]    [Pg.241]    [Pg.277]    [Pg.279]    [Pg.283]    [Pg.304]    [Pg.321]    [Pg.345]    [Pg.124]    [Pg.1061]    [Pg.76]    [Pg.99]    [Pg.108]    [Pg.163]    [Pg.176]    [Pg.233]    [Pg.234]    [Pg.241]    [Pg.279]    [Pg.283]    [Pg.304]    [Pg.321]    [Pg.1111]    [Pg.351]    [Pg.473]    [Pg.229]    [Pg.2289]    [Pg.64]    [Pg.201]    [Pg.236]    [Pg.248]    [Pg.509]   
See also in sourсe #XX -- [ Pg.216 ]



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