吡喹酮在诱导和未诱导大鼠肝微粒体内的羟化代谢概貌及其羟化物的质谱鉴定  被引量：2

作　　者：张渝娟[1] 全钰珠[1] 黄婉芸[1] 

机构地区：[1]重庆医科大学药理教研室

出　　处：《中国药理学与毒理学杂志》1996年第1期56-61,共6页Chinese Journal of Pharmacology and Toxicology

摘　　要：用细胞色素Ｐ４５０（Ｐ４５０）特异诱导剂研究参与吡喹酮（ＰＱＴ）代谢的Ｐ４５０同工酶，在未诱导肝微粒体内，ＰＱＴ代谢仅生成其Ｄ环单羟化物．在β－萘黄酮诱导肝微粒体内，ＰＱＴ代谢后也生成其Ｄ环单羟化物．ＰＱＴ在苯巴比妥诱导的肝微粒体内代谢生成Ｄ环，Ｂ环和Ａ环三个单羟化物．在地塞米松和红霉素诱导的肝微粒体内，ＰＱＴ代谢生成七个代谢产物．结果表明参与ＰＱＴ分子羟化的Ｐ４５０同工酶至少包括ＣＹＰ１Ａ，ＣＹＰ２Ｂ和ＣＹＰ３Ａ亚家族，每个亚家族代谢ＰＱＴ的概貌各不相同，ＣＹＰ３Ａ优先羟化Ａ环，ＣＹＰ２Ｂ优先羟化Ｄ环和Ｂ环，ＣＹＰ１Ａ则几乎仅羟化Ｄ环．The cytochrome P450(P450) isoforms which might be responsible for the hydroxylation of PQT were investigated in rat liver microsomes by using P450 specific inducers. After PQT was incubated with untreated or CYP1A inducer β-NF treated rat liver microsomes, only one major metabolite was found from high performance liquid chromatogram. Mass spectrum showed that both of them were D-Ring monohydroxylate. The content of P450 and the formation rate of PQT D-Ring monohydroxylate in liver microsomes with pretreatment of β-NF was enhanced to 1 55 and 2 12 fold respectively as compared with that in the control. In the CYP2B inducer PB treated rat liver microsomes, the content of P450 was enhanced to 4 31 fold. Three major metabolites were found after PQT incubated with the PB induced microsomes. Mass spectra showed that they were PQT D-Ring, B-Ring and A-Ring monohydroxylated products and the formation rate of D-Ring monohydroxylate was 6 05 fold increased. In liver microsomes obtained from rats pretreated with DEX, the CYP3A inducer, P450 content was increased about 2 69 fold. Seven PQT hydroxylated metabolites, including one D-Ring, two B-Rings, one A-Ring, one C-Ring position 1 and one position 11b monohydroxylate and one D- and B-ring dihydroxylate were found. The formation rate of D-Ring monohydroxylate was increased to 1 94 fold. These results suggest that at least three subfamilies CYP1A, CYP2B and CYP3A are involved in the metablism of PQT. Metabolic profile of PQT is different in different specific inducer pretreated microsomes. CYP3A preferentially catalyzes A-Ring, CYP2B preferentially cytalyzes D-Ring and B-Ring hydroxylation, while CYP1A seems to catalyze D-Ring hydroxylation only in our study conditions.

关 键 词：抗蠕虫药 吡喹酮 肝代谢 代谢 质谱测定 

分 类 号：R978.63[医药卫生—药品] R969.1[医药卫生—药学]