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雄性F344大鼠肝脏增生性结节中细胞色素P450 mRNA表达及相关类固醇羟化活性降低。

Decreased expression of cytochrome P450 mRNAs and related steroid hydroxylation activities in hepatic hyperplastic nodules in male F344 rats.

作者信息

Chen Z Y, White C C, Eaton D L

机构信息

Department of Environmental Health, University of Washington, Seattle 98195.

出版信息

Toxicol Appl Pharmacol. 1993 Nov;123(1):151-9. doi: 10.1006/taap.1993.1232.

Abstract

To explore the mechanism(s) underlying the relationship between expression of cytochrome P450 (CYP) enzymes and growth of hepatic hyperplastic nodules, mRNA of CYP1A1, 1A2, 2B1, 2B2, 2C6, 2C11, and 3A1, and CYP enzyme-mediated hydroxylation of testosterone (T), 17 beta-estradiol (E), and corticosterone (C) were determined in a group of selected large nodules from livers of male F344 rats given the modified Solt-Farber resistance protocol and compared with control and surrounding tissue. Slot-blot analysis with specific oligonucleotides showed little or no mRNA of CYP2B1, 2B2, and 2C6 in nodules, surrounding tissue, and control liver without PB treatment. Constitutive expression of CYP1A2, 2C11, and 3A1 in nodules was from 2 to 10 times less in nodules than in control liver. BP treatment increased mRNA of CYP2B1, 2B2, 2C6, 2C11, and 3A1 in control and surrounding tissue substantially, but was 3 to 11 times less in the nodules than in the control liver. Messenger RNA of CYP1A1 was not detected in either nodules or control livers independent of PB treatment. HPLC determination demonstrated a general pattern of a decrease in CYP enzyme-mediated hydroxylation of T, E, and C in the nodules relative to the surrounding tissue and control liver. The differences between nodules and control liver were usually 3 to 10-fold for the 12 metabolites detected although smaller decreases were observed for a few metabolites in some nodules. PB increased the rate of hydroxylation for 11 of the 12 metabolites and resulted in 2 additional metabolites of both T and E in control liver and some nodules. However, the general pattern of lower hydroxylation activities in the nodules relative to the surrounding tissue remained the same as that in the non-PB group. These observations are consistent with the hypothesis that intracellular kinetics of endogenous CYP enzyme substrates may differ in some nodules, relative to the surrounding tissue, as a result of decreased expression of CYP genes. This difference in CYP expression pattern in turn may contribute to the selective growth and progression to cancer of certain nodules, as many endogenous CYP enzyme substrates are modulators of DNA and RNA synthesis and cellular growth and differentiation.

摘要

为探究细胞色素P450(CYP)酶表达与肝增生性结节生长之间关系的潜在机制,在一组经改良的Solt-Farber抗性方案处理的雄性F344大鼠肝脏中选取的大结节中,测定了CYP1A1、1A2、2B1、2B2、2C6、2C11和3A1的mRNA,以及CYP酶介导的睾酮(T)、17β-雌二醇(E)和皮质酮(C)的羟化作用,并与对照和周围组织进行比较。用特异性寡核苷酸进行的狭缝印迹分析显示,在未用苯巴比妥(PB)处理的结节、周围组织和对照肝脏中,CYP2B1、2B2和2C6的mRNA很少或未检测到。结节中CYP1A2、2C11和3A1的组成型表达比对照肝脏低2至10倍。PB处理使对照和周围组织中CYP2B1、2B2、2C6、2C11和3A1的mRNA显著增加,但在结节中的表达比对照肝脏低3至11倍。无论是否进行PB处理,在结节或对照肝脏中均未检测到CYP1A1的信使核糖核酸。高效液相色谱测定表明,相对于周围组织和对照肝脏,结节中CYP酶介导的T、E和C的羟化作用总体呈下降趋势。尽管在一些结节中少数代谢物的下降幅度较小,但所检测的12种代谢物在结节与对照肝脏之间的差异通常为3至10倍。PB增加了12种代谢物中11种的羟化速率,并在对照肝脏和一些结节中产生了另外2种T和E的代谢物。然而,结节中相对于周围组织较低的羟化活性总体模式与非PB组相同。这些观察结果与以下假设一致:由于CYP基因表达降低,内源性CYP酶底物的细胞内动力学在某些结节中可能与周围组织不同。CYP表达模式的这种差异反过来可能有助于某些结节的选择性生长和向癌症的进展,因为许多内源性CYP酶底物是DNA和RNA合成以及细胞生长和分化的调节剂。

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