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首页> 外文期刊>Archives of Toxicology >Differential alterations in levels of hepatic microsomal cytochrome P450 isozymes following intracerebroventricular injection of bacterial lipopolysaccharide in rats.
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Differential alterations in levels of hepatic microsomal cytochrome P450 isozymes following intracerebroventricular injection of bacterial lipopolysaccharide in rats.

机译:肝微粒体细胞色素分子淋巴脑膜血管脂多糖肝硬化后肝微粒体细胞色素P450型水平的差异改变。

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To investigate the effect of central inflammation due to bacterial infection, such as meningitis, on the activities of hepatic cytochromes P450 (CYPs), rats were injected intracerebroventricularly (i.c.v.) with 0.1 microg of bacterial lipopolysaccharide (LPS). The LPS i.c.v. injection significantly decreased the total P450 contents (by 30% of the levels of control rats treated with saline i.c.v.), the contents of CYP1A (48%), 2B (54%), 2C11 (37%) and 3A (40%) and related drug metabolizing activities, 7-ethoxycoumarin O-deethylation (36%), imipramine N-demethylation (41%) and erythromycin N-demethylation (33%) in liver microsomes 24 h after the treatment. In contrast, intraperitoneal (i.p.) injection of LPS at the same dose as i.c.v. (0.1 microg) did not significantly affect the hepatic microsomal contents of total P450 or the content of each individual CYP isozyme and its activity. CYP2D1 protein and the activity of imipramine 2-hydroxylase were not significantly decreased by LPS injection regardless of the route of administration. The inhibitory effects of 0.1 microg i.c.v. LPS on the activities of these CYPs were almost equal to those of 10 microg i.p. LPS, and 0.01 microg of i.c.v. LPS significantly decreased the activity of imipramine N-demethylase only. Therefore, the LPS i.c.v. injection resulted in CYP isozyme-selective inhibition at an ineffective dose when injected i.p.. It is suggested that a central inflammation, such as meningitis, differentially decreases the levels of hepatic CYP isozymes. A possible involvement is discussed of the central nervous system in this down-regulation.
机译:为了探讨中枢炎症因细菌感染的影响,例如脑膜炎,肝细胞学P450(CYPS)的活性,大鼠脑内(I.C.V.)注射0.1微米的细菌脂多糖(LPS)。 lps i.c.v.注射显着降低了总P450含量(用盐水ICV处理的对照大鼠水平的30%),CYP1A(48%),2B(54%),2C11(37%)和3A(40%)和3A(40%)的含量在治疗后24小时,相关药物代谢活性,7-乙氧基苏马林O-脱甲酰化(36%),含氨基氨基氨基(41%)和红霉素N-去甲基化(33%)。相反,腹膜内(I.P.)以与I.C.V相同的剂量注射LPS。 (0.1 microg)没有显着影响总P450的肝微粒体或每种CYP同工酶的含量及其活性。无论施用途径如何,LPS注射都不会显着降低CYP2D1蛋白和含丙氨酸2-羟化酶的活性。 0.1 microg i.c.v的抑制作用。 LPS对这些CYP的活动几乎等于10 microg i.p. LPS,和0.01微孔I.C.V. LPS仅显着降低了含染色N-脱甲酶的活性。因此,LPS I.C.V.注射导致CYP同工酶选择性抑制在无效剂量时,当注射I.P中。建议,诸如脑膜炎的中枢炎症差异降低肝CYP同工酶的水平。在该下调中讨论了中枢神经系统的可能参与。

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