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人类谷胱甘肽 S-转移酶 A(GSTA)家族基因受类固醇生成因子 1(SF-1)调控,参与类固醇生成。

Human glutathione S-transferase A (GSTA) family genes are regulated by steroidogenic factor 1 (SF-1) and are involved in steroidogenesis.

机构信息

Department of Biochemistry, Faculty of Medical Sciences, University of Fukui, Shimoaizuki, Matsuoka, Eiheiji, Fukui 910-1193, Japan.

出版信息

FASEB J. 2013 Aug;27(8):3198-208. doi: 10.1096/fj.12-222745. Epub 2013 May 6.

DOI:10.1096/fj.12-222745
PMID:23650189
Abstract

Steroidogenic factor 1 (SF-1) is a master regulator for steroidogenesis. In this study, we identified novel SF-1 target genes using a genome-wide promoter tiling array and a DNA microarray. SF-1 was found to regulate human glutathione S-transferase A (GSTA) family genes (hGSTA1-hGSTA4), a superfamily of detoxification enzymes clustered on chromosome 6p12. All hGSTA genes were up-regulated by transduction of SF-1 into human mesenchymal stem cells, while knockdown of endogenous SF-1 in H295R cells down-regulated all hGSTA genes. Chromatin immunoprecipitation assays, however, revealed that SF-1 bound directly to the promoters of hGSTA3 and weakly of hGSTA4. Chromosome conformation capture assays revealed that the coordinated expression of the genes was based on changes in higher-order chromatin structure triggered by SF-1, which enables the formation of long-range interactions, at least between hGSTA1 and hGSTA3 gene promoters. In steroidogenesis, dehydrogenation of the 3-hydroxy group and subsequent Δ(5)-Δ(4) isomerization are thought to be enzymatic properties of 3β-hydroxysteroid dehydrogenase (3β-HSD). Here, we demonstrated that, in steroidogenic cells, the hGSTA1 and hGSTA3 gene products catalyze Δ(5)-Δ(4) isomerization in a coordinated fashion with 3β-HSD II to produce progesterone or Δ(4)-androstenedione from their Δ(5)-precursors. Thus, hGSTA1 and hGSTA3 gene products are new members of steroidogenesis working as Δ(5)-Δ(4) isomerases.

摘要

固醇生成因子 1(SF-1)是类固醇生成的主要调节因子。在这项研究中,我们使用全基因组启动子平铺阵列和 DNA 微阵列鉴定了新的 SF-1 靶基因。SF-1 被发现调节人类谷胱甘肽 S-转移酶 A(GSTA)家族基因(hGSTA1-hGSTA4),这是一组位于 6p12 染色体上的解毒酶超家族。将 SF-1 转导到人骨髓间充质干细胞中会导致所有 hGSTA 基因上调,而在 H295R 细胞中敲低内源性 SF-1 会下调所有 hGSTA 基因。然而,染色质免疫沉淀试验显示 SF-1 直接结合到 hGSTA3 和 hGSTA4 基因的启动子上。染色质构象捕获试验表明,基因的协调表达基于 SF-1 触发的高级染色质结构变化,这使得长距离相互作用形成,至少在 hGSTA1 和 hGSTA3 基因启动子之间形成。在类固醇生成中,3-羟基的脱氢和随后的 Δ(5)-Δ(4)异构化被认为是 3β-羟甾脱氢酶(3β-HSD)的酶学特性。在这里,我们证明在类固醇生成细胞中,hGSTA1 和 hGSTA3 基因产物与 3β-HSD II 协同催化 Δ(5)-Δ(4)异构化,从其 Δ(5)-前体物生成孕酮或 Δ(4)-雄烯二酮。因此,hGSTA1 和 hGSTA3 基因产物是作为 Δ(5)-Δ(4)异构酶参与类固醇生成的新成员。

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