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雌激素受体α异构体通过隐匿外显子的选择性使用产生。

Estrogen Receptor α Isoforms Generated by Alternative Use of Cryptic Exons.

机构信息

Department of Anatomy and Neurobiology, Graduate School of Medicine, Nippon Medical School.

出版信息

J Nippon Med Sch. 2023 Nov 7;90(5):364-371. doi: 10.1272/jnms.JNMS.2023_90-507. Epub 2023 Aug 8.

DOI:10.1272/jnms.JNMS.2023_90-507
PMID:37558429
Abstract

Estrogen receptor α (ERα) regulates several physiological functions. In pathophysiological conditions, ERα is involved in the development and progression of estrogen-sensitive tumors. The ERα gene contains multiple 5'-untranslated exons and eight conventional coding exons and presents multiple isoforms generated by alternative promoter usage and alternative splicing. This gene also possesses non-conventional exons in the 3'- and intronic regions, and alternative use of cryptic exons contributes to further diversity of ERα mRNAs and proteins. Recently, the genomic organization of ERα genes and the splicing profiles of their transcripts were comparatively analyzed in humans, mice, and rats, and multiple ERα isoforms with distinct structures and functions were identified. These transcripts contain cryptic sequences that encode insertion-containing or truncated ERα proteins. In particular, alternative cryptic exons with in-frame stop codons yield transcripts encoding C-terminally-truncated ERα proteins. The C-terminally-truncated ERα isoforms lack part or all of the ligand-binding domain but possess an isoform-specific sequence. Some of these isoforms exhibit constitutive transactivation and resistance to estrogen receptor antagonists. Although numerous studies have reported conflicting results regarding their functions, the critical determinant for their gain-of-function has been identified structurally. Here we review recent progress in ERα variant research concerning the genomic organization of ERα genes, splicing profiles of ERα transcripts, and transactivation properties of ERα isoforms.

摘要

雌激素受体 α(ERα)调节多种生理功能。在病理生理条件下,ERα参与雌激素敏感肿瘤的发生和发展。ERα 基因包含多个 5′非翻译外显子和八个常规编码外显子,并通过不同启动子的使用和选择性剪接产生多种异构体。该基因在 3′和内含子区域还具有非传统外显子,而隐蔽外显子的选择性使用有助于 ERα mRNA 和蛋白质的进一步多样化。最近,对人类、小鼠和大鼠的 ERα 基因的基因组组织和转录本的剪接谱进行了比较分析,确定了具有不同结构和功能的多种 ERα 异构体。这些转录本包含编码插入型或截断型 ERα 蛋白的隐蔽序列。特别是,具有无义终止密码子的选择性隐蔽外显子产生编码 C 末端截断 ERα 蛋白的转录本。C 末端截断的 ERα 异构体缺乏部分或全部配体结合域,但具有异构体特异性序列。其中一些异构体表现出组成型反式激活和对雌激素受体拮抗剂的抗性。尽管许多研究报告了关于其功能的相互矛盾的结果,但它们获得功能的关键决定因素在结构上已被确定。在这里,我们综述了关于 ERα 基因的基因组组织、ERα 转录本的剪接谱以及 ERα 异构体的反式激活特性的 ERα 变体研究的最新进展。

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