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假定的人类α重组热点的证据和特征

Evidence and characteristics of putative human alpha recombination hotspots.

作者信息

Zhang Jing, Li Fei, Li Jun, Zhang Michael Q, Zhang Xuegong

机构信息

MOE Key laboratory of Bioinformatics, Department of Automation, Tsinghua University, Bejing, China.

出版信息

Hum Mol Genet. 2004 Nov 15;13(22):2823-8. doi: 10.1093/hmg/ddh310. Epub 2004 Sep 22.

Abstract

Understanding recombination rate variation is very important for studying genome diversity and evolution, and for investigation of phenotypic association and genetic diseases. Recombination hotspots have been observed in many species and are well studied in yeast. Recent study demonstrated that recombination hotspots are also a ubiquitous feature of the human genome. But the nature of human hotspots remains largely unknown. We have developed and validated a novel computational method for testing the existence of hotspots as well as for localizing them with either unphased or phased genotyping data. To study the characteristics of hotspots within or close to genes, we scanned for unusually high levels of recombination using the European population samples in the SeattleSNPs database, and found evidence for the existence of human alpha hotspots similar to those of yeast. This type of hotspots, found at promoter regions, accounts for about half of the total detected and appears to depend on some specific transcription factor binding sites (such as CGCCCCCGC). These characteristics can explain the observed weak correlation between hotspots and GC-content, and their variation may contribute to the diversity of hotspot distribution among different individuals and species. These long-sought putative human alpha recombination hotspots should deserve further experimental investigations.

摘要

了解重组率变异对于研究基因组多样性和进化,以及调查表型关联和遗传疾病非常重要。在许多物种中都观察到了重组热点,并且在酵母中对其进行了深入研究。最近的研究表明,重组热点也是人类基因组的一个普遍特征。但是人类热点的本质在很大程度上仍然未知。我们已经开发并验证了一种新的计算方法,用于测试热点的存在以及使用未分型或分型的基因分型数据对其进行定位。为了研究基因内部或附近热点的特征,我们使用西雅图SNP数据库中的欧洲人群样本扫描了异常高水平的重组,并发现了与酵母类似的人类α热点存在的证据。这种在启动子区域发现的热点类型约占检测到的总数的一半,并且似乎依赖于一些特定的转录因子结合位点(如CGCCCCCGC)。这些特征可以解释观察到的热点与GC含量之间的弱相关性,并且它们的变异可能导致不同个体和物种之间热点分布的多样性。这些长期寻找的假定人类α重组热点值得进一步的实验研究。

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