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人类重复序列L1家族的亚家族结构与进化

Subfamily structure and evolution of the human L1 family of repetitive sequences.

作者信息

Jurka J

机构信息

Linus Pauling Institute of Science and Medicine, Palo Alto, California 94306.

出版信息

J Mol Evol. 1989 Dec;29(6):496-503. doi: 10.1007/BF02602921.

Abstract

Comparative analysis of the available 3'-portions of the human L1 (LINE-1) family of repeated sequences indicates that all the sequences can be classified in two major subfamilies. The division is based on patterns of diagnostic bases shared within L1 subfamilies of sequences but differing between them. The overall ratio of replacement to synonymous positions, occupied by the diagnostic bases in the large open reading frame of the L1 sequence, is 1.15. This indicates that both subfamilies were obtained from genes coding for functional proteins. The L1 subfamilies appear to be of different ages and may represent a "fossil record" of the same active gene at different times in the history of primates. The younger subfamily can be split further into at least two closely related branches of sequences. The above facts combined with the recent data for the Alu subfamily structure show that LINE and SINE families of interspersed repeats share discontinuous patterns in their evolution. These data are consistent with the model that both Alu and L1 families, as well as other pseudogene families, contain active genes producing discrete layers of pseudogenes throughout the history of primates. Models of evolutionary processes that could generate these discontinuities are discussed together with the possible biological role of Alu and L1 genes.

摘要

对人类L1(长散在核元件1)重复序列家族现有3'端部分的比较分析表明,所有序列可分为两个主要亚家族。这种划分基于L1序列亚家族内部共享但彼此不同的诊断性碱基模式。L1序列大的开放阅读框中诊断性碱基占据的替换与同义位点的总体比率为1.15。这表明两个亚家族均源自编码功能蛋白的基因。L1亚家族似乎具有不同的年代,可能代表灵长类动物历史上不同时期同一活性基因的“化石记录”。较年轻的亚家族可进一步细分为至少两个密切相关的序列分支。上述事实与最近关于Alu亚家族结构的数据相结合,表明散布重复序列的LINE和SINE家族在其进化过程中具有不连续模式。这些数据与以下模型一致,即Alu和L1家族以及其他假基因家族在灵长类动物的整个历史中都包含产生离散假基因层的活性基因。文中讨论了可能产生这些不连续性的进化过程模型以及Alu和L1基因可能的生物学作用。

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