CLINICAL PHARMACOKINETICS OF RIFABUTIN

被引：56

作者：

SKINNER, MH ^{[1
]}

BLASCHKE, TF ^{[1
]}

机构：

[1] STANFORD UNIV,MED CTR,DIV CLIN PHARMACOL,STANFORD,CA 94305

来源：

CLINICAL PHARMACOKINETICS | 1995年 / 28卷 / 02期

关键词：

D O I：

10.2165/00003088-199528020-00003

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The clinical effectiveness of rifabutin for prophylaxis of disseminated Mycobacterium avium complex infection has recently been demonstrated in HIV-positive patients with low CD4 counts. Rifabutin is a newly marketed, semisynthetic antimycobacterial agent similar to rifampicin (rifampin) in structure and activity. However, rifabutin has important pharmacokinetic differences compared with rifampicin. Rifabutin has relatively low oral bioavailability; about 20% after single dose administration. With long term administration rifabutin induces its own metabolism and the metabolism of some other drugs. The elimination half-life of rifabutin is long (45 hours) but, as a result of a very large volume of distribution (>9 L/kg), average plasma concentrations remain relatively low after repeated administration of standard doses. In vitro rifabutin is more active against M. avium-intracellulare complex and at least as active against M. tuberculosis as rifampicin. In vivo the advantage of rifabutin is less apparent due to its lower plasma concentrations at equivalent doses. Adverse effects are unusual at the recommended oral dosage of 300 mg/day, but become common as the total daily dose approaches 1 g. Dose-limiting toxicity consists of a polyarthralgia/arthritis syndrome, possibly complicated by uveitis. More clinical studies are needed to establish the role of rifabutin in combination therapy for M. avium-intracellulare complex and other mycobacterial infections.

引用

页码：115 / 125

页数：11

共 77 条

[1] ABSORPTION, DISPOSITION AND PRELIMINARY METABOLIC PATHWAY OF C-14 RIFABUTIN IN ANIMALS AND MAN [J].

BATTAGLIA, R ;

PIANEZZOLA, E ;

SALGAROLLO, G ;

ZINI, G ;

BENEDETTI, MS .

JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY, 1990, 26 (06) :813-822

[2] AUTOINDUCTION OF RIFABUTIN METABOLISM IN MAN [J].

BENEDETTI, MS ;

EFTHYMIOPOULOS, C ;

SASSELLA, D ;

MORO, E ;

REPETTO, M .

XENOBIOTICA, 1990, 20 (11) :1113-1119

[3]

BENEDETTI MS, 1993, 9 INT C AIDS BERL, V1, P501

[4] PARTITION DATA OF PENICILLINS DETERMINED BY MEANS OF REVERSED-PHASE THIN-LAYER CHROMATOGRAPHY [J].

BIAGI, GL ;

BARBARO, AM ;

GAMBA, MF ;

GUERRA, MC .

JOURNAL OF CHROMATOGRAPHY, 1969, 41 (3-4) :371-&

[5]

Breda M., 1992, Drug Metabolism and Drug Interactions, V10, P323

[6] THE EARLY BACTERICIDAL ACTIVITY OF RIFABUTIN MEASURED BY SPUTUM VIABLE COUNTS IN HONG-KONG PATIENTS WITH PULMONARY TUBERCULOSIS [J].

CHAN, SL ;

YEW, WW ;

MA, WK ;

GIRLING, DJ ;

ABER, VR ;

FELMINGHAM, D ;

ALLEN, BW ;

MITCHISON, DA .

TUBERCLE AND LUNG DISEASE, 1992, 73 (01) :33-38

[7] ANTIMICROBIAL ACTIVITY OF RIFABUTIN IN COMBINATION WITH 2 AND 3 OTHER ANTIMICROBIAL AGENTS AGAINST STRAINS OF MYCOBACTERIUM-PARATUBERCULOSIS [J].

CHIODINI, RJ .

JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY, 1991, 27 (02) :171-176

[8] URINARY METABOLITES OF RIFABUTIN, A NEW ANTIMYCOBACTERIAL AGENT, IN HUMAN VOLUNTEERS [J].

COCCHIARA, G ;

BENEDETTI, MS ;

VICARIO, GP ;

BALLABIO, M ;

GIOIA, B ;

VIOGLIO, S ;

VIGEVANI, A .

XENOBIOTICA, 1989, 19 (07) :769-780

[9] COMPARATIVE INVITRO ACTIVITIES OF MDL 473, RIFAMPIN, AND ANSAMYCIN AGAINST MYCOBACTERIUM-INTRACELLULARE [J].

CYNAMON, MH .

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1985, 28 (03) :440-441

[10] RIFABUTIN IN COMBINATION WITH CLOFAZIMINE, ISONIAZID AND ETHAMBUTOL IN THE TREATMENT OF AIDS PATIENTS WITH INFECTIONS DUE TO OPPORTUNIST MYCOBACTERIA [J].

DAUTZENBERG, B ;

TRUFFOT, C ;

MIGNON, A ;

ROZENBAUM, W ;

KATLAMA, C ;

PERRONNE, C ;

PARROT, R ;

GROSSET, J .

TUBERCLE, 1991, 72 (03) :168-175

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