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首页> 外文期刊>Molecular phylogenetics and evolution >Gene turnover and differential retention in the relaxin/insulin-like gene family in primates
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Gene turnover and differential retention in the relaxin/insulin-like gene family in primates

机译:灵长类动物松弛素/胰岛素样基因家族中的基因更新和差异保留

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The relaxin/insulin-like gene family is related to the insulin gene family, and includes two separate types of peptides: relaxins (RLNs) and insulin-like peptides (INSLs) that perform a variety of physiological roles including testicular descent, growth and differentiation of the mammary glands, trophoblast development, and cell differentiation. In vertebrates, these genes are found on three separate genomic loci, and in mammals, variation in the number and nature of genes in this family is mostly restricted to the Relaxin Family Locus B. For example, this locus contains a single copy of RLN in platypus and opossum, whereas it contains copies of the INSL6, INSL4, RLN2 and RLN1 genes in human and chimp. The main objective of this research is to characterize changes in the size and membership composition of the RLN/INSL gene family in primates, reconstruct the history of the RLN/INSL genes of primates, and test competing evolutionary scenarios regarding the origin of INSL4 and of the duplicated copies of the RLN gene of apes. Our results show that the relaxin/INSL-like gene family of primates has had a more dynamic evolutionary history than previously thought, including several examples of gene duplications and losses which are consistent with the predictions of the birth-and-death model of gene family evolution. In particular, we found that the differential retention of relatively old paralogs played a key role in shaping the gene complement of this family in primates. Two examples of this phenomenon are the origin of the INSL4 gene of catarrhines (the group that includes Old World monkeys and apes), and of the duplicate RLN1 and RLN2 paralogs of apes. In the case of INSL4, comparative genomics and phylogenetic analyses indicate that the origin of this gene, which was thought to represent a catarrhine-specific evolutionary innovation, is as old as the split between carnivores and primates, which took place approximately 97 million years ago. In addition, in the case of the RLN1 and RLN2 genes of apes our phylogenetic trees and topology tests indicate that the duplication that gave rise to these two genes maps to the last common ancestor of anthropoid primates. All these genomic changes in gene complement, which are particularly prevalent among anthropoid primates, might be linked to the many physiological and anatomical changes found in this group. Given the various roles of members of the RLN/INSL-like gene family in reproductive biology, it might be that changes in this gene family are associated to changes in reproductive traits.
机译:松弛素/胰岛素样基因家族与胰岛素基因家族有关,包括两种独立类型的肽:松弛素(RLN)和胰岛素样肽(INSL),它们执行各种生理作用,包括睾丸下降,生长和分化乳腺,滋养细胞发育和细胞分化。在脊椎动物中,这些基因存在于三个单独的基因组位点上,而在哺乳动物中,该家族中基因的数量和性质的变异主要限于Relaxin家族基因座B。例如,该基因座仅包含一个RLN拷贝。鸭嘴兽和负鼠,而它包含人类和黑猩猩中INSL6,INSL4,RLN2和RLN1基因的副本。这项研究的主要目的是表征灵长类动物RLN / INSL基因家族的大小和成员组成的变化,重建灵长类动物RLN / INSL基因的历史,并测试关于INSL4和INSL4起源的竞争性进化方案。猿的RLN基因的重复副本。我们的结果表明,灵长类动物的Relaxin / INSL样基因家族比以前认为的具有更动态的进化历史,其中包括一些基因重复和缺失的例子,这些例子与基因家族的生死模型的预测相符。演化。特别是,我们发现相对较旧的同系物的差异保留在塑造灵长类中该家族的基因补体中起关键作用。这种现象的两个例子是卡他汀的INSL4基因(包括古猿和猿类)的起源以及猿类RLN1和RLN2重复的同源物。就INSL4而言,比较基因组学和系统发育分析表明,该基因的起源被认为代表卡他碱特异性进化创新,其起源与食肉动物和灵长类动物的分裂一样古老,这种分裂发生于大约9,700万年前。 。此外,对于猿类的RLN1和RLN2基因,我们的系统树和拓扑测试表明,导致这两个基因重复的基因映射到类人猿灵长类动物的最后共同祖先。所有这些基因补体的基因组变化,特别是在类人猿灵长类动物中普遍存在,可能与这一组的许多生理和解剖学变化有关。鉴于RLN / INSL样基因家族成员在生殖生物学中的各种作用,该基因家族的改变可能与生殖性状的改变有关。

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