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紫杉醇对原代培养人肝细胞中细胞色素P4503A的诱导作用。

Induction of cytochrome P4503A by taxol in primary cultures of human hepatocytes.

作者信息

Kostrubsky V E, Lewis L D, Strom S C, Wood S G, Schuetz E G, Schuetz J D, Sinclair P R, Wrighton S A, Sinclair J F

机构信息

Veterans Administration Medical Center, White River Junction, Vermont, 05009, USA.

出版信息

Arch Biochem Biophys. 1998 Jul 15;355(2):131-6. doi: 10.1006/abbi.1998.0730.

Abstract

In primary cultures of human hepatocytes, paclitaxel (Taxol), at pharmacological concentrations, was demonstrated to induce immunoreactive cytochrome P4503A (CYP3A). The magnitude of the inductive response of the hepatocytes to Taxol varied in five separate cultures. In general, exposure to increasing concentrations of Taxol (0.2 to 10 microM) resulted in increases in immunoreactive CYP3A. In four of the cultures, treatment of hepatocytes with the lowest concentration of Taxol tested (0.2 microM) resulted in approximately two-fold increases in CYP3A. In the other culture, however, a six-fold increase in CYP3A was observed at 0.2 microM. Taxol was almost as effective as rifampicin in inducing CYP3A in two of the cultures, but less effective than rifampicin in two other cultures. CYP3A4 mRNA was increased by Taxol. Increases in CYP3A4 mRNA correlated with increases in the levels of immunoreactive CYP3A. These results demonstrate that Taxol is a potent inducer of CYP3A in human hepatocytes. The clinical significance of these findings is discussed.

摘要

在原代培养的人肝细胞中,药理学浓度的紫杉醇(泰素)可诱导免疫反应性细胞色素P4503A(CYP3A)。在五个独立的培养物中,肝细胞对紫杉醇的诱导反应程度有所不同。一般来说,暴露于浓度不断增加的紫杉醇(0.2至10微摩尔)会导致免疫反应性CYP3A增加。在其中四个培养物中,用测试的最低浓度紫杉醇(0.2微摩尔)处理肝细胞导致CYP3A增加约两倍。然而,在另一个培养物中,在0.2微摩尔时观察到CYP3A增加了六倍。在其中两个培养物中,紫杉醇诱导CYP3A的效果几乎与利福平相同,但在另外两个培养物中则不如利福平有效。紫杉醇可增加CYP3A4 mRNA。CYP3A4 mRNA的增加与免疫反应性CYP3A水平的增加相关。这些结果表明,紫杉醇是人类肝细胞中CYP3A的有效诱导剂。讨论了这些发现的临床意义。

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