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眼部发育中替代启动子的使用:转录因子MITF的复杂作用与调控

Alternative promoter use in eye development: the complex role and regulation of the transcription factor MITF.

作者信息

Bharti Kapil, Liu Wenfang, Csermely Tamas, Bertuzzi Stefano, Arnheiter Heinz

机构信息

Mammalian Development Section, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Development. 2008 Mar;135(6):1169-78. doi: 10.1242/dev.014142. Epub 2008 Feb 13.

Abstract

During vertebrate eye development, the transcription factor MITF plays central roles in neuroepithelial domain specification and differentiation of the retinal pigment epithelium. MITF is not a single protein but represents a family of isoforms generated from a common gene by alternative promoter/exon use. To address the question of the role and regulation of these isoforms, we first determined their expression patterns in developing mouse eyes and analyzed the role of some of them in genetic models. We found that two isoforms, A- and J-Mitf, are present throughout development in both retina and pigment epithelium, whereas H-Mitf is detected preferentially and D-Mitf exclusively in the pigment epithelium. We further found that a genomic deletion encompassing the promoter/exon regions of H-, D- and B-Mitf leads to novel mRNA isoforms and proteins translated from internal start sites. These novel proteins lack the normal, isoform-specific N-terminal sequences and are unable to support the development of the pigment epithelium, but are capable of inducing pigmentation in the ciliary margin and the iris. Moreover, in mutants of the retinal Mitf regulator Chx10 (Vsx2), reduced cell proliferation and abnormal pigmentation of the retina are associated with a preferential upregulation of H- and D-Mitf. This retinal phenotype is corrected when H- and D-Mitf are missing in double Mitf/Chx10 mutants. The results suggest that Mitf regulation in the developing eye is isoform-selective, both temporally and spatially, and that some isoforms, including H- and D-Mitf, are more crucial than others in effecting normal retina and pigment epithelium development.

摘要

在脊椎动物眼睛发育过程中,转录因子小眼畸形相关转录因子(MITF)在神经上皮区域特化和视网膜色素上皮细胞分化中发挥核心作用。MITF并非单一蛋白质,而是由一个共同基因通过选择性启动子/外显子使用产生的一组同工型蛋白。为了探究这些同工型蛋白的作用和调控机制,我们首先确定了它们在发育中小鼠眼睛中的表达模式,并分析了其中一些在遗传模型中的作用。我们发现,两种同工型蛋白A-Mitf和J-Mitf在视网膜和色素上皮细胞的整个发育过程中均有表达,而H-Mitf主要在色素上皮细胞中被检测到,D-Mitf仅在色素上皮细胞中表达。我们进一步发现,一个包含H-Mitf、D-Mitf和B-Mitf启动子/外显子区域的基因组缺失导致了从内部起始位点翻译的新型mRNA同工型和蛋白质。这些新型蛋白质缺乏正常的、同工型特异性的N端序列,无法支持色素上皮细胞的发育,但能够诱导睫状体边缘和虹膜色素沉着。此外,在视网膜MITF调节因子Chx10(Vsx2)的突变体中,视网膜细胞增殖减少和色素沉着异常与H-Mitf和D-Mitf的优先上调有关。当双突变体Mitf/Chx10中缺失H-Mitf和D-Mitf时,这种视网膜表型得到纠正。结果表明,发育中的眼睛中MITF的调控在时间和空间上具有同工型选择性,并且一些同工型蛋白,包括H-Mitf和D-Mitf,在影响正常视网膜和色素上皮细胞发育方面比其他同工型更为关键。

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