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跗猴线粒体基因组中的控制区长度动态变化可能驱动氨基酸进化。

Control region length dynamics potentially drives amino acid evolution in tarsier mitochondrial genomes.

作者信息

Merker Stefan, Thomas Sarah, Völker Elke, Perwitasari-Farajallah Dyah, Feldmeyer Barbara, Streit Bruno, Pfenninger Markus

机构信息

Department of Zoology, State Museum of Natural History Stuttgart, Rosenstein 1, 70191, Stuttgart, Germany,

出版信息

J Mol Evol. 2014 Aug;79(1-2):40-51. doi: 10.1007/s00239-014-9631-2. Epub 2014 Jul 10.

Abstract

Patterns and processes of molecular evolution critically influence inferences in phylogeny and phylogeography. Within primates, a shift in evolutionary rates has been identified as the rationale for contrasting findings from mitochondrial and nuclear DNA studies as to the position of Tarsius. While the latter now seems settled, we sequenced complete mitochondrial genomes of three Sulawesi tarsiers (Tarsius dentatus, T. lariang, and T. wallacei) and analyzed substitution rates among tarsiers and other primates to infer driving processes of molecular evolution. We found substantial length polymorphism of the D-loop within tarsier individuals, but little variation of predominant lengths among them, regardless of species. Length variation was due to repetitive elements in the CSB domain-minisatellite motifs of 35 bp length and microsatellite motifs of 6 bp length. Amino acid evolutionary rates were second highest among major primate taxa relative to nucleotide substitution rates. We observed many radical possibly function-altering amino acid changes that were rarely driven by positive selection and thus potentially slightly deleterious or neutral. We hypothesize that the observed pattern of an increased amino acid evolutionary rate in tarsier mitochondrial genomes may be caused by hitchhiking of slightly deleterious mutations with favored D-loop length variants selected for maximizing replication success within the cell or the mitochondrion.

摘要

分子进化的模式和过程对系统发育学和系统地理学的推断有着至关重要的影响。在灵长类动物中,进化速率的转变被认为是线粒体和核DNA研究在眼镜猴位置上得出不同结果的原因。虽然后者现在似乎已经确定,但我们对三只苏拉威西眼镜猴(德氏眼镜猴、拉氏眼镜猴和华莱士眼镜猴)的线粒体基因组进行了测序,并分析了眼镜猴与其他灵长类动物之间的替代率,以推断分子进化的驱动过程。我们发现眼镜猴个体内D环存在大量长度多态性,但无论物种如何,它们之间主要长度的差异很小。长度变异是由于CSB结构域中的重复元件——35bp长度的小卫星基序和6bp长度的微卫星基序。相对于核苷酸替代率,氨基酸进化速率在主要灵长类分类群中排第二高。我们观察到许多可能改变功能的激进氨基酸变化,这些变化很少由正选择驱动,因此可能具有轻微的有害性或中性。我们假设,在眼镜猴线粒体基因组中观察到的氨基酸进化速率增加的模式,可能是由于轻微有害突变与为在细胞或线粒体内最大化复制成功而选择的有利D环长度变体的搭便车效应所致。

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