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小鼠和大鼠肝脏及肠道中细胞色素P450介导的代谢比较。

Comparison of mouse and rat cytochrome P450-mediated metabolism in liver and intestine.

作者信息

Martignoni Marcella, Groothuis Geny, de Kanter Ruben

机构信息

Preclinical Development, Nerviano Medical Sciences, Viale Pasteur 10, 20014 Nerviano (MI), Italy.

出版信息

Drug Metab Dispos. 2006 Jun;34(6):1047-54. doi: 10.1124/dmd.105.009035. Epub 2006 Mar 24.

Abstract

The liver is considered to be the major site of first-pass metabolism, but the small intestine is also able to contribute significantly. The improvement of existing in vitro techniques and the development of new ones, such as intestinal slices, allow a better understanding of the intestine as a metabolic organ. In this paper, the formation of metabolites of several human CYP3A substrates by liver and intestinal slices from rat and mouse was compared. The results show that liver slices exhibited a higher metabolic rate for the majority of the studied substrates, but some metabolites were produced at a higher rate by intestinal slices, compared with liver slices. Coincubation with ketoconazole inhibited the metabolic conversion in intestinal slices almost completely, but inhibition was variable in liver slices. To better understand the role of CYP3A in mice, we studied the relative mRNA expression of different CYP3A isoforms in intestine and liver from mice because, in this species, CYP3A expression has not been well described in these organs. It was found that in mice, CYP3A13 is more expressed in the intestine, whereas CYP3A11, CYP3A25, and CYP3A41 are more expressed in the liver, comparable to similar findings in the rat. Altogether, these data demonstrate that, in addition to liver, the intestine from mouse and rat may have an important role in the process of first-pass metabolism, depending on the substrate. Moreover, we show that intestinal slices are a useful in vitro technique to study gut metabolism.

摘要

肝脏被认为是首过代谢的主要部位,但小肠也能发挥重要作用。现有体外技术的改进以及新方法(如肠切片)的发展,使人们能更好地了解小肠作为代谢器官的功能。本文比较了大鼠和小鼠肝脏及肠切片对几种人CYP3A底物代谢产物的形成情况。结果表明,对于大多数研究的底物,肝脏切片表现出更高的代谢率,但与肝脏切片相比,有些代谢产物在肠切片中的生成速率更高。与酮康唑共同孵育几乎完全抑制了肠切片中的代谢转化,但在肝脏切片中的抑制作用则有所不同。为了更好地了解CYP3A在小鼠中的作用,我们研究了小鼠肠和肝脏中不同CYP3A亚型的相对mRNA表达,因为在这个物种中,这些器官中CYP3A的表达情况尚未得到充分描述。研究发现,在小鼠中,CYP3A13在肠道中表达较多,而CYP3A11、CYP3A25和CYP3A41在肝脏中表达较多,这与在大鼠中的类似发现相当。总之,这些数据表明除肝脏外,小鼠和大鼠的肠道在首过代谢过程中可能根据底物发挥重要作用。此外,我们表明肠切片是研究肠道代谢的一种有用的体外技术。

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