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人类Y染色体雄性特异区域的染色体间基因转换模式

Patterns of Inter-Chromosomal Gene Conversion on the Male-Specific Region of the Human Y Chromosome.

作者信息

Trombetta Beniamino, D'Atanasio Eugenia, Cruciani Fulvio

机构信息

Dipartimento di Biologia e Biotecnologie "Charles Darwin", Sapienza Università di RomaRome, Italy.

Istituto di Biologia e Patologia Molecolari, Consiglio Nazionale delle Ricerche (CNR),Rome, Italy.

出版信息

Front Genet. 2017 May 3;8:54. doi: 10.3389/fgene.2017.00054. eCollection 2017.

Abstract

The male-specific region of the human Y chromosome (MSY) is characterized by the lack of meiotic recombination and it has long been considered an evolutionary independent region of the human genome. In recent years, however, the idea that human MSY did not have an independent evolutionary history begun to emerge with the discovery that inter-chromosomal gene conversion (ICGC) can modulate the genetic diversity of some portions of this genomic region. Despite the study of the dynamics of this molecular mechanism in humans is still in its infancy, some peculiar features and consequences of it can be summarized. The main effect of ICGC is to increase the allelic diversity of MSY by generating a significant excess of clustered single nucleotide polymorphisms (SNPs) (defined as groups of two or more SNPs occurring in close proximity and on the same branch of the Y phylogeny). On the human MSY, 13 inter-chromosomal gene conversion hotspots (GCHs) have been identified so far, involving donor sequences mainly from the X-chromosome and, to a lesser extent, from autosomes. Most of the GCHs are evolutionary conserved and overlap with regions involved in aberrant X-Y crossing-over. This review mainly focuses on the dynamics and the current knowledge concerning the recombinational landscape of the human MSY in the form of ICGC, on how this molecular mechanism may influence the evolution of the MSY, and on how it could affect the information enclosed within a genomic region which, until recently, appeared to be an evolutionary independent unit.

摘要

人类Y染色体的男性特异性区域(MSY)的特点是缺乏减数分裂重组,长期以来它一直被认为是人类基因组中一个进化上独立的区域。然而近年来,随着染色体间基因转换(ICGC)能够调节该基因组区域某些部分的遗传多样性这一发现,人类MSY没有独立进化历史的观点开始出现。尽管对人类这种分子机制动态的研究仍处于起步阶段,但可以总结出它的一些独特特征和后果。ICGC的主要作用是通过产生大量过量的成簇单核苷酸多态性(SNP)(定义为在Y系统发育的同一分支上紧密相邻出现的两个或更多SNP组)来增加MSY的等位基因多样性。在人类MSY上,目前已鉴定出13个染色体间基因转换热点(GCH),其供体序列主要来自X染色体,在较小程度上也来自常染色体。大多数GCH在进化上是保守的,并且与异常X-Y交叉互换所涉及的区域重叠。本综述主要关注以ICGC形式存在的人类MSY重组格局的动态和当前知识,这种分子机制如何影响MSY的进化,以及它如何影响一个直到最近似乎还是进化独立单元的基因组区域内所包含的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ae27/5413550/5479f6cb8557/fgene-08-00054-g001.jpg

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