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机构地区:[1]重庆医科大学药理教研室
出 处:《药学学报》1997年第1期5-10,共6页Acta Pharmaceutica Sinica
摘 要:三乙酰竹桃霉素(TAO)可使地塞米松(DEX)诱导的大鼠肝微粒体内未结合细胞色素P450(P450)含量降低,红霉素(ERY)和乙基吗啡(EMP)N脱甲基酶活性降低和吡喹酮(PZQ)A环一羟化物生成速率降低。TAO和ERY对PZQA环一羟化物的生成表现为竟争性抑制,且PZQA环一羟化物生成速率与ERY,EMPN脱甲基酶活性高度相关。结果表明,P4503A(CYP3A)参与了PZQA环的羟化。The possibility of involvement of cytochrome P4503A(CYP3A) in the monohydroxylation of the ring A of praziquantel(PZQ) was studied by using CYP3A specific inducer dexamethasone(DEX), specific inhibitor triacetyloeandomycin(TAO) and the activity of erythromycin(ERY) and ethylmorphine(EMP) N demethylase which are known to be marker for CYP3A enzyme activity as probes. In the liver microsomes obtained from rats pretreated with CYP3A inducer DEX with TAO treatment the content of uncomplexed P450 was decreased, the activity of ERY and EMP N demethylase was reduced, and simultaneously, the rate of formation of ring A monohydroxylate of PZQ was inhibited. Ring A monohydroxylate formation was competitively inhibited by TAO and ERY. The rates of ring A monohydroxylate formation were strongly correlated with the activity of N demethylase of ERY and EMP. These results indicate that CYP3A is involved in the monohydroxylation of the ring A of PZQ.
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