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核糖体RNA的祖先插入和扩增并不支持核糖体起源于其肽基转移酶中心的观点。

Ancestral Insertions and Expansions of rRNA do not Support an Origin of the Ribosome in Its Peptidyl Transferase Center.

作者信息

Caetano-Anollés Gustavo

机构信息

Evolutionary Bioinformatics Laboratory, Department of Crop Sciences, University of Illinois at Urbana-Champaign, Urbana, IL, 61801, USA,

出版信息

J Mol Evol. 2015 Apr;80(3-4):162-5. doi: 10.1007/s00239-015-9677-9. Epub 2015 Apr 12.

DOI:10.1007/s00239-015-9677-9
PMID:25864085
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4555209/
Abstract

Phylogenetic reconstruction of ribosomal history suggests that the ribonucleoprotein complex originated in structures supporting RNA decoding and ribosomal mechanics. A recent study of accretion of ancestral expansion segments of rRNA, however, contends that the large subunit of the ribosome originated in its peptidyl transferase center (PTC). Here I re-analyze the rRNA insertion data that supports this claim. Analysis of a crucial three-way junction connecting the long-helical coaxial branch that supports the PTC to the L1 stalk and its translocation functions reveals an incorrect branch-to-trunk insertion assignment that is in conflict with the PTC-centered accretion model. Instead, the insertion supports the ancestral origin of translocation. Similarly, an insertion linking a terminal coaxial trunk that holds the L7-12 stalk and its GTPase center to a seven-way junction of the molecule again questions the early origin of the PTC. Unwarranted assumptions, dismissals of conflicting data, structural insertion ambiguities, and lack of phylogenetic information compromise the construction of an unequivocal insertion-based model of macromolecular accretion. Results prompt integration of phylogenetic and structure-based models to address RNA junction growth and evolutionary constraints acting on ribosomal structure.

摘要

核糖体历史的系统发育重建表明,核糖核蛋白复合体起源于支持RNA解码和核糖体机制的结构。然而,最近一项关于rRNA祖先扩展片段积累的研究认为,核糖体的大亚基起源于其肽基转移酶中心(PTC)。在此,我重新分析了支持这一观点的rRNA插入数据。对连接支持PTC的长螺旋同轴分支与L1茎及其转位功能的关键三向连接点的分析揭示了一个错误的分支到主干的插入分配,这与以PTC为中心的积累模型相冲突。相反,该插入支持转位的祖先起源。同样,一个将持有L7 - 12茎及其GTP酶中心的末端同轴主干与分子的七向连接点相连的插入再次对PTC的早期起源提出质疑。无根据的假设、对冲突数据的忽视、结构插入的模糊性以及缺乏系统发育信息,都损害了基于插入的明确大分子积累模型的构建。结果促使将系统发育和基于结构的模型相结合,以解决RNA连接点生长和作用于核糖体结构的进化限制问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/736d/4555209/a980332f1aa1/239_2015_9677_Fig1_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/736d/4555209/a980332f1aa1/239_2015_9677_Fig1_HTML.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/736d/4555209/a980332f1aa1/239_2015_9677_Fig1_HTML.jpg

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