共 38 条
Mechanism-based inactivation of CYP450 enzymes: a case study of lapatinib
被引:25
作者:

Ho, Han Kiat
论文数: 0 引用数: 0
h-index: 0
机构:
Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore

Chan, James Chun Yip
论文数: 0 引用数: 0
h-index: 0
机构:
Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore

Hardy, Klarissa D.
论文数: 0 引用数: 0
h-index: 0
机构:
Lipscomb Univ, Coll Pharm, Nashville, TN USA Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore

Chan, Eric Chun Yong
论文数: 0 引用数: 0
h-index: 0
机构:
Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore
机构:
[1] Natl Univ Singapore, Dept Pharm, Fac Sci, Singapore 117543, Singapore
[2] Lipscomb Univ, Coll Pharm, Nashville, TN USA
基金:
美国国家卫生研究院;
关键词:
CYP3A;
drug-drug interaction;
lapatinib;
mechanism-based inactivation;
toxicity;
METASTATIC BREAST-CANCER;
CYTOCHROME-P450;
3A4;
DEPENDENT INHIBITION;
INDUCED HEPATITIS;
TIENILIC ACID;
PHASE-I;
METABOLISM;
CYP3A4;
DRUG;
THERAPY;
D O I:
10.3109/03602532.2014.1003648
中图分类号:
R9 [药学];
学科分类号:
1007 ;
摘要:
Mechanism-based inactivation (MBI) of CYP450 enzymes is a unique form of inhibition in which the enzymatic machinery of the victim is responsible for generation of the reactive metabolite. This precondition sets up a time-dependency for the inactivation process, a hallmark feature that characterizes all MBI. Yet, MBI itself is a complex biochemical phenomenon that operates in different modes, namely, covalent binding to apoprotein, covalent binding of the porphyrin group and also complexation of the catalytic iron. Using lapatinib as a recent example of toxicological interest, we present an example of a mixed-function MBI that can confound clinical drug-drug interactions manifestation. Lapatinib exhibits both covalent binding to the apoprotein and formation of a metabolite-intermediate complex in an enzyme-selective manner (CYP3A4 versus CYP3A5), each with different reactive metabolites. The clinical implication of this effect is also contingent upon genetic polymorphisms of the enzyme involved as well as the co-administration of other substrates, inhibitors or inducers, culminating in drug-drug interactions. This understanding recapitulates the importance of applying isoform-specific mechanistic investigations to develop customized strategies to manage such outcomes.
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页码:21 / 28
页数:8
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