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同源转录因子的功能分化支持棘皮动物生物矿化的进化。

Functional divergence of paralogous transcription factors supported the evolution of biomineralization in echinoderms.

机构信息

Department of Biological Sciences, Carnegie Mellon University, Pittsburgh, United States.

出版信息

Elife. 2017 Nov 20;6:e32728. doi: 10.7554/eLife.32728.

Abstract

Alx1 is a pivotal transcription factor in a gene regulatory network that controls skeletogenesis throughout the echinoderm phylum. We performed a structure-function analysis of sea urchin Alx1 using a rescue assay and identified a novel, conserved motif (Domain 2) essential for skeletogenic function. The paralogue of Alx1, Alx4, was not functionally interchangeable with Alx1, but insertion of Domain 2 conferred robust skeletogenic function on Alx4. We used cross-species expression experiments to show that Alx1 proteins from distantly related echinoderms are not interchangeable, although the sequence and function of Domain 2 are highly conserved. We also found that Domain 2 is subject to alternative splicing and provide evidence that this domain was originally gained through exonization. Our findings show that a gene duplication event permitted the functional specialization of a transcription factor through changes in exon-intron organization and thereby supported the evolution of a major morphological novelty.

摘要

Alx1 是一个关键的转录因子,存在于一个调控整个棘皮动物门骨骼发生的基因调控网络中。我们利用拯救实验对海胆 Alx1 进行了结构-功能分析,并鉴定出一个新的、保守的基序(结构域 2),该基序对骨骼发生功能至关重要。Alx1 的同源物 Alx4 不能与 Alx1 进行功能互换,但插入结构域 2 可赋予 Alx4 强大的骨骼发生功能。我们利用跨物种表达实验表明,尽管结构域 2 的序列和功能高度保守,但来自亲缘关系较远的棘皮动物的 Alx1 蛋白不能互换。我们还发现结构域 2 可进行选择性剪接,并提供证据表明该结构域最初是通过外显子化获得的。我们的研究结果表明,基因复制事件通过改变外显子-内含子组织,使转录因子的功能专业化,从而支持了主要形态新颖性的进化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/65a4/5758115/17946107ca32/elife-32728-fig1.jpg

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