The Human Membrane Progesterone Receptor Gene: Genomic Structure and Promoter Analysis

Sabine Bernauer, M. Wehling, Dirk Gerdes And, E. Falkenstein
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引用次数: 28

Abstract

Rapid, nongenomic effects of steroids are likely to be mediated by membrane receptors not by intracellular steroid receptors. We recently identified a progesterone membrane binding protein (mPR) from human liver. The corresponding hmpr gene is comprised of 3 exons and 2 introns. The promoter sequence of hmpr lacks a typical TATA box but contains instead a high homology to a transcription Initiatior consensus sequence, which overlaps the experimentally determined transcriptional start site. The major proximal promoter is GC-rich and sequence analysis revealed a CpG island spanning the transcriptional start site. Several putative cis-regulatory DNA-motifs, which represent possible binding sites for transcription factors like AP2, NF-AT, Ahr/Arnt and C/EBP were identified in the genomic upstream region by sequence homology. Functional analysis of differently deleted fragments of the hmpr upstream region in a GFP-reportergene assay in transiently transfected cultured cells indicates the general testability of the hmpr promoter in vivo.
人膜孕酮受体基因:基因组结构和启动子分析
类固醇的快速非基因组效应可能是由膜受体介导的,而不是由细胞内类固醇受体介导的。我们最近从人肝脏中鉴定出一种黄体酮膜结合蛋白(mPR)。相应的hmpr基因由3个外显子和2个内含子组成。hmpr的启动子序列缺乏典型的TATA盒,但包含与转录起始一致序列的高度同源性,该序列与实验确定的转录起始位点重叠。主要的近端启动子富含gc,序列分析显示一个CpG岛横跨转录起始位点。通过序列同源性,在基因组上游区域鉴定了几个推测的顺式调控dna基序,它们代表了AP2、NF-AT、Ahr/Arnt和C/EBP等转录因子的可能结合位点。在瞬时转染的培养细胞中,gfp报告基因实验对hmpr上游区域不同缺失片段的功能分析表明,hmpr启动子在体内具有一般的可测试性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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