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Ribosomal frameshifting and transcriptional slippage: From genetic steganography and cryptography to adventitious use

机译:核糖体移码和转录滑移:从遗传隐写术和密码术到不定式使用

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摘要

Genetic decoding is not ‘frozen’ as was earlier thought, but dynamic. One facet of this is frameshifting that often results in synthesis of a C-terminal region encoded by a new frame. Ribosomal frameshifting is utilized for the synthesis of additional products, for regulatory purposes and for translational ‘correction’ of problem or ‘savior’ indels. Utilization for synthesis of additional products occurs prominently in the decoding of mobile chromosomal element and viral genomes. One class of regulatory frameshifting of stable chromosomal genes governs cellular polyamine levels from yeasts to humans. In many cases of productively utilized frameshifting, the proportion of ribosomes that frameshift at a shift-prone site is enhanced by specific nascent peptide or mRNA context features. Such mRNA signals, which can be 5′ or 3′ of the shift site or both, can act by pairing with ribosomal RNA or as stem loops or pseudoknots even with one component being 4 kb 3′ from the shift site. Transcriptional realignment at slippage-prone sequences also generates productively utilized products encoded trans-frame with respect to the genomic sequence. This too can be enhanced by nucleic acid structure. Together with dynamic codon redefinition, frameshifting is one of the forms of recoding that enriches gene expression.
机译:遗传解码不是像以前认为的那样“冻结”,而是动态的。其中一个方面是移码,通常会导致合成由新帧编码的C端区域。核糖体移码可用于合成其他产品,用于监管目的以及用于翻译“校正”问题或“救星”插入缺失。在移动染色体元件和病毒基因组的解码中,主要用于合成其他产物。一类稳定染色体基因的调节移码控制着细胞多胺水平(从酵母到人类)。在许多有效利用移码的情况下,特定新生肽或mRNA上下文特征会增加在移频位点移码的核糖体比例。这样的mRNA信号可以是转移位点的5'或3',或两者都可以通过与核糖体RNA配对或作为茎环或假结来起作用,即使其中一个成分距离转移位点3'为4 kb。易滑序列的转录重排也产生了相对于基因组序列反式编码的生产性利用产物。这也可以通过核酸结构来增强。与动态密码子重新定义一起,移码是丰富基因表达的重新编码形式之一。

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