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对Xp22.3上一组硫酸酯酶基因的特征分析表明,在一个祖先假常染色体区域存在基因重复。

Characterization of a cluster of sulfatase genes on Xp22.3 suggests gene duplications in an ancestral pseudoautosomal region.

作者信息

Meroni G, Franco B, Archidiacono N, Messali S, Andolfi G, Rocchi M, Ballabio A

机构信息

Telethon Institute of Genetics and Medicine (TIGEM), Milano, Italy.

出版信息

Hum Mol Genet. 1996 Apr;5(4):423-31. doi: 10.1093/hmg/5.4.423.

Abstract

An obligatory crossing-over event between the X and Y chromosomes in mammals occurs at each male meiosis within the 2.6 Mb of DNA defining the pseudoautosomal region (PAR). Genes located within or near the human PAR have homologous copies on the X and Y chromosomes, escape X inactivation and appear to be highly divergent throughout evolution. We have characterized the genomic structure of two genes from a recently identified cluster of sulfatase genes (ARSD and ARSE) located in the Xp22.3 region, and of their homologs on the Y chromosome. Our results indicate that the ARSD and ARSE genes from within this cluster have a conserved genomic organization, shared also by another Xp22.3 gene, STS, but completely different from that of all the other sulfatase genes. Sequence analysis of the Y-linked homologs indicate that they represent truncated pseudogenes. Sequence identity values between the X and Y copies of each gene is on average 91%, significantly higher than the values obtained by comparing different members of the family. FISH mapping experiments performed in several primate species revealed an identical localization of the X-linked copies to that in man, but different localizations of the Y homologs. Together, our data indicate that the cluster of sulfatase genes on human Xp22.3 was created through duplication events which probably occurred in an ancestral PAR, and support the view that the PAR has undergone multiple changes during recent mammalian evolution.

摘要

哺乳动物中,X和Y染色体之间的强制性交叉事件发生在每个雄性减数分裂过程中,位于界定拟常染色体区域(PAR)的2.6 Mb DNA范围内。位于人类PAR内或附近的基因在X和Y染色体上有同源拷贝,逃避X染色体失活,并且在整个进化过程中似乎高度分化。我们已经对位于Xp22.3区域的一个最近鉴定出的硫酸酯酶基因簇(ARSD和ARSE)中的两个基因及其在Y染色体上的同源物的基因组结构进行了表征。我们的结果表明,该基因簇中的ARSD和ARSE基因具有保守的基因组组织,另一个Xp22.3基因STS也具有这种组织,但与所有其他硫酸酯酶基因的基因组组织完全不同。对Y连锁同源物的序列分析表明它们代表截短的假基因。每个基因的X和Y拷贝之间的序列同一性值平均为91%,显著高于通过比较该家族不同成员获得的值。在几种灵长类物种中进行的荧光原位杂交定位实验显示,X连锁拷贝的定位与人类相同,但Y同源物的定位不同。总之,我们的数据表明,人类Xp22.3上的硫酸酯酶基因簇是通过可能发生在祖先PAR中的重复事件形成的,并支持这样一种观点,即PAR在最近的哺乳动物进化过程中经历了多次变化。

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