METABOLISM AND METABOLITE PHARMACOKINETICS OF BRB-I-28, A CLASS IB ANTIARRHYTHMIC AGENT

被引：12

作者：

CHEN, CL

SANGIAH, S

BOURNE, DWA

RODER, JD

CHEN, H

ALAVI, FK

CLARKE, CR

GARRISON, GL

BERLIN, KD

COUCH, KM

ZISMAN, SA

SCHERLAG, BJ

LAZZARA, R

VANDERHELM, D

机构：

[1] OKLAHOMA STATE UNIV,COLL VET MED,DEPT PHYSIOL SCI,STILLWATER,OK 74078

[2] OKLAHOMA STATE UNIV,DEPT CHEM,STILLWATER,OK 74078

[3] UNIV OKLAHOMA,VET AFFAIRS MED CTR,HLTH SCI CTR,OKLAHOMA CITY,OK

[4] UNIV OKLAHOMA,DEPT CHEM,NORMAN,OK 73019

来源：

EUROPEAN JOURNAL OF DRUG METABOLISM AND PHARMACOKINETICS | 1995年 / 20卷 / 02期

关键词：

BRB-I-28; ANTIARRHYTHMICS; METABOLISM;

D O I：

10.1007/BF03226370

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The metabolism of BRB-I-28 (7-benzyl-3-thia-7-azabicyclo[3.3.1]nonane), a novel class Ib antiarrhythmic agent, was characterized in vivo in dogs and rats and in vitro with rat liver microsomal preparations containing a NADPH-generating system. In dogs, rats and the in vitro hepatic microsomal oxidation system, BRB-I-28 was extensively metabolized to form 7-benzyl-3-thia-7-azabicyclo[3.3.1]nonane-3-oxide (I), a major metabolite. The metabolite I was produced via S-oxidation, presumably by the hepatic P-450 system. Formation of a minor metabolite, 7-benzoyl-3-thia-7-azabicyclo[3.3.1]nonane (II) via the oxidation of the benzylic site was also identified in rats. Following intravenous and oral administration of BRB-I-28 to dogs, the plasma concentration of major metabolite I could be best described by a I-compartmental model. The plasma AUC of metabolite I was 20% (i.v.) and 179.4% (oral) of that of the parent BRB-I-28, respectively, suggesting that BRB-I-28 was metabolized significantly by the first pass effect following oral administration. Extensive metabolism of BRB-I-28 to form metabolites I and II, which have demonstrated much lower antiarrhythmic activities, further supports previously observed pharmacodynamic and pharmacokinetic findings.

引用

页码：151 / 161

页数：11

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