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Alu 衍生的旧世界猴外显子化事件和 LEPR 基因的实验验证。

Alu-derived old world monkeys exonization event and experimental validation of the LEPR gene.

机构信息

National Primate Research Center, Korea Research Institute of Bioscience and Biotechnology, Ochang, 363-883, Korea.

出版信息

Mol Cells. 2010 Sep;30(3):201-7. doi: 10.1007/s10059-010-0108-x. Epub 2010 Aug 23.

DOI:10.1007/s10059-010-0108-x
PMID:20803091
Abstract

The leptin receptor (LEPR) is a crucial regulatory protein that interacts with Leptin. In our analysis of LEPR, novel AluJb-derived alternative transcripts were identified in the genome of the rhesus monkey. In order to investigate the occurrence of AluJb-derived alternative transcripts and the mechanism underlying exonization events, we conducted analyses using a number of primate genomic DNAs and adipose RNAs of tissue and primary cells derived from the crab-eating monkey. Our results demonstrate that the AluJb element has been integrated into our common ancestor genome prior to the divergence of simians and prosimians. The lineage-specific exonization event of the LEPR gene in chimpanzees, orangutans, and Old World monkeys appear to have been accomplished via transition mutations of the 5' splicing site (second position of C to T). However, in New World monkeys and prosimians, the AluJb-related LEPR transcript should be silenced by the additional transversion mutation (fourth position of T to G). The AluJb-related transcript of human LEPR should also be silenced by a mutation of the 5' splicing site (first position of G to A) and the insertion of one nucleotide sequence (minus fourth position of A). Our data suggests that lineage-specific exonization events should be determined by the combination event of the formation of splicing sites and protection against site-specific mutation pressures. These evolutionary mechanisms could be major sources for primate diversification.

摘要

瘦素受体(LEPR)是一种与瘦素相互作用的关键调节蛋白。在我们对 LEPR 的分析中,在恒河猴的基因组中鉴定出了新型 AluJb 衍生的选择性转录本。为了研究 AluJb 衍生的选择性转录本的发生和外显子化事件的机制,我们使用了一些灵长类动物基因组 DNA 和源自食蟹猴的组织和原代细胞的脂肪 RNA 进行了分析。我们的结果表明,AluJb 元件在灵长类动物和原猴类动物分化之前就已经整合到我们的共同祖先基因组中。黑猩猩、猩猩和旧世界猴 LEPR 基因的谱系特异性外显子化事件似乎是通过 5'剪接位点(C 到 T 的第二位)的转换突变完成的。然而,在新世界猴和原猴中,AluJb 相关的 LEPR 转录本应该通过额外的颠换突变(T 到 G 的第四位)而被沉默。人类 LEPR 的 AluJb 相关转录本也应该通过 5'剪接位点(G 到 A 的第一位)的突变和一个核苷酸序列的插入(减去 A 的第四位)而被沉默。我们的数据表明,谱系特异性外显子化事件应该由剪接位点的形成和对特定突变压力的保护的组合事件决定。这些进化机制可能是灵长类动物多样化的主要来源。

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