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海胆类hbox12/pmar1/micro1多基因家族的时空表达多样化及拷贝数变异

Diversification of spatiotemporal expression and copy number variation of the echinoid hbox12/pmar1/micro1 multigene family.

作者信息

Cavalieri Vincenzo, Geraci Fabiana, Spinelli Giovanni

机构信息

Department of Biological, Chemical and Pharmaceutical Sciences and Technologies (STEBICEF), University of Palermo, Viale delle Scienze Edificio 16, Palermo, Italy.

Advanced Technologies Network Center (ATeN), University of Palermo, Viale delle Scienze Edificio 18, Palermo, Italy.

出版信息

PLoS One. 2017 Mar 28;12(3):e0174404. doi: 10.1371/journal.pone.0174404. eCollection 2017.

Abstract

Changes occurring during evolution in the cis-regulatory landscapes of individual members of multigene families might impart diversification in their spatiotemporal expression and function. The archetypal member of the echinoid hbox12/pmar1/micro1 family is hbox12-a, a homeobox-containing gene expressed exclusively by dorsal blastomeres, where it governs the dorsal/ventral gene regulatory network during embryogenesis of the sea urchin Paracentrotus lividus. Here we describe the inventory of the hbox12/pmar1/micro1 genes in P. lividus, highlighting that gene copy number variation occurs across individual sea urchins of the same species. We show that the various hbox12/pmar1/micro1 genes group into three subfamilies according to their spatiotemporal expression, which ranges from broad transcription throughout development to transient expression in either the animal hemisphere or micromeres of the early embryo. Interestingly, the promoter regions of those genes showing comparable expression patterns are highly similar, while differing from those of the other subfamilies. Strikingly, phylogenetic analysis suggests that the hbox12/pmar1/micro1 genes are species-specific, exhibiting extensive divergence in their noncoding, but not in their coding, sequences across three distinct sea urchin species. In spite of this, two micromere-specific genes of P. lividus possess a TCF/LEF-binding motif in a similar position, and their transcription relies on Wnt/β-catenin signaling, similar to the pmar1 and micro1 genes, which in other sea urchin species are involved in micromere specification. Altogether, our findings suggest that the hbox12/pmar1/micro1 gene family evolved rather rapidly, generating paralogs whose cis-regulatory sequences diverged following multiple rounds of duplication from a common ancestor.

摘要

多基因家族中各个成员的顺式调控格局在进化过程中发生的变化,可能会使其时空表达和功能产生多样化。海胆类hbox12/pmar1/micro1家族的原型成员是hbox12-a,这是一个含同源异型框的基因,仅由背侧卵裂球表达,在海胆Paracentrotus lividus胚胎发生过程中,它调控背/腹基因调控网络。在此,我们描述了Paracentrotus lividus中hbox12/pmar1/micro1基因的情况,强调同一物种的不同海胆个体间存在基因拷贝数变异。我们发现,各种hbox12/pmar1/micro1基因根据其时空表达可分为三个亚家族,其表达范围从整个发育过程中的广泛转录到早期胚胎动物半球或小分裂球中的瞬时表达。有趣的是,那些显示出相似表达模式的基因的启动子区域高度相似,而与其他亚家族的启动子区域不同。引人注目的是,系统发育分析表明,hbox12/pmar1/micro1基因是物种特异性的,在三种不同海胆物种的非编码序列中表现出广泛的差异,但编码序列没有差异。尽管如此,Paracentrotus lividus的两个小分裂球特异性基因在相似位置具有一个TCF/LEF结合基序,并且它们的转录依赖于Wnt/β-连环蛋白信号传导,这与pmar1和micro1基因相似,在其他海胆物种中,pmar1和micro1基因参与小分裂球的特化。总之,我们的研究结果表明,hbox12/pmar1/micro1基因家族进化相当迅速,产生了旁系同源基因,其顺式调控序列在从共同祖先经过多轮复制后发生了分歧。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/42a1/5370098/d16e63b06db4/pone.0174404.g001.jpg

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