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升高的bax/bcl-2比值与前列腺上皮细胞凋亡的发生相对应。

An elevated bax/bcl-2 ratio corresponds with the onset of prostate epithelial cell apoptosis.

作者信息

Perlman H, Zhang X, Chen M W, Walsh K, Buttyan R

机构信息

The Department of Urology,The College of Physicians and Surgeons of Columbia University, Atchley Pavilion 11th Floor, 161 Fort Washington Blvd., New York, NY 10032, USA.

出版信息

Cell Death Differ. 1999 Jan;6(1):48-54. doi: 10.1038/sj.cdd.4400453.

Abstract

The prostate gland in adult male rats is highly dependent on androgenic steroids. Castration initiates the regression of this tissue through a process involving the loss of the vast majority of cells by means of apoptosis. We studied this well characterized in vivo model of apoptosis to evaluate how the expression of two particular gene products, bcl-2 and bax, known to be important for the regulation of apoptosis were affected by castration. An RNase protection assay designed to quantify the levels of bax mRNA showed that this transcript was transiently elevated after castration, reaching a peak in expression at 3 days and declining thereafter. In contrast, bcl-2 mRNA expression was continuously elevated over a period of up to 7 days after castration. The distinct changes in the expression of the mRNAs encoding these two genes were confirmed by an in situ hybridization analysis of regressing rat ventral prostate tissues. The elevation in mRNAs were apparently restricted to the secretory epithelial cells of the gland, the cellular compartment of the tissue most affected by castration. Finally, SDS - PAGE/Western blot analysis of bax and bcl-2 protein expression in the regressing rat prostate gland with bax and bcl-2-specific antibodies showed that the changes in the bax and bcl-2 protein levels were similar and consistent to that found for the mRNAs. In summary, the expression of both bax and bcl-2 gene products are uniquely modulated during castration-induced regression of the rat ventral prostate gland. The changes we observed identify a transient but marked increase in the bax/bcl-2 expression ratio of the tissue that peaks on the second and third days after castration, coinciding with the peak periods of prostate cell apoptosis. These data support previous studies done on in vitro systems wherein it was shown that the bax/bcl-2 ratio determines the apoptotic potential of a cell.

摘要

成年雄性大鼠的前列腺高度依赖雄激素类固醇。阉割通过一个涉及绝大多数细胞通过凋亡而丧失的过程启动该组织的退化。我们研究了这个特征明确的体内凋亡模型,以评估已知对凋亡调节很重要的两种特定基因产物bcl-2和bax的表达如何受到阉割的影响。一种旨在定量bax mRNA水平的核糖核酸酶保护分析表明,该转录本在阉割后短暂升高,在第3天达到表达峰值,此后下降。相反,bcl-2 mRNA表达在阉割后长达7天的时间内持续升高。通过对退化的大鼠腹侧前列腺组织进行原位杂交分析,证实了编码这两个基因的mRNA表达的明显变化。mRNA的升高显然局限于腺体的分泌上皮细胞,这是组织中受阉割影响最大的细胞区室。最后,用bax和bcl-2特异性抗体对退化的大鼠前列腺中bax和bcl-2蛋白表达进行SDS - PAGE/蛋白质印迹分析表明,bax和bcl-2蛋白水平的变化与mRNA的变化相似且一致。总之,在阉割诱导的大鼠腹侧前列腺退化过程中,bax和bcl-2基因产物的表达都受到独特的调节。我们观察到的变化表明,组织的bax/bcl-2表达比值在阉割后第二和第三天达到峰值,出现短暂但显著的增加,这与前列腺细胞凋亡的高峰期一致。这些数据支持了先前在体外系统中进行的研究,该研究表明bax/bcl-2比值决定细胞的凋亡潜力。

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