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Alignment-based and alignment-free methods converge with experimental data on amino acids coded by stop codons at split between nuclear and mitochondrial genetic codes

机译:基于对准和对准的方法将通过在核和线粒体遗传码之间分离的终止密码子编码的氨基酸的实验数据收敛

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摘要

Genetic codes mainly evolve by reassigning punctuation codons, starts and stops. Previous analyses assuming that undefined amino acids translate stops showed greater diveigence between nuclear and mitochondrial genetic codes. Here, three independent methods converge on which amino acids translated stops at split between nuclear and mitochondrial genetic codes: (a) alignment-free genetic code comparisons inserting different amino acids at stops; (b) alignment-based blast analyses of hypothetical peptides translated from non-coding mitochondrial sequences, inserting different amino acids at stops; (c) biases in amino acid insertions at stops in proteomic data. Hence short-term protein evolution models reconstruct long-term genetic code evolution. Mitochondria reassign stops to amino acids otherwise inserted at stops by codon-anticodon mismatches (near-cognate tRNAs). Hence dual function (translation termination and translation by codon-anticodon mismatch) precedes mitochondrial reassignments of stops to amino acids Stop ambiguity increases coded information, compensates endocellular mitogenome reduction. Mitochondrial codon leassignments might prevent viral infections. (c) 2018 Elsevier B.V. All rights reserved.
机译:遗传密码主要通过重新分配标点来分区,开始和停止来发展。先前的分析假设未定义的氨基酸转化止动术在核和线粒体遗传码之间表现出更大的脱位。这里,三种独立方法会聚在核和线粒体遗传码之间的分裂中翻译的氨基酸:(a)对准的遗传码比较在止挡时插入不同氨基酸的比较; (b)从非编码线粒体序列翻译的假设肽的基于对准的爆炸分析,在止挡时插入不同的氨基酸; (c)蛋白质组学数据中氨基酸插入的偏置。因此,短期蛋白质演进模型重建长期遗传码演化。线粒体重新分配到诸如Codon-Antodon失配(近同源TrNAS)的停止时被插入氨基酸。因此,双重功能(通过Codon-Antodon Mismatch的翻译终止和翻译)之前对氨基酸的停止止动液的线粒体重新分配止动模糊性增加了编码信息,补偿了内皮细胞介导的减少。线粒体密码子释放剂可能预防病毒感染。 (c)2018 Elsevier B.v.保留所有权利。

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