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Protospacer recognition motifs: Mixed identities and functional diversity

机译:Protospacer识别主题:混合身份和功能多样性

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摘要

Protospacer adjacent motifs (PAMs) were originally characterized for CRISPR-Cas systems that were classified on the basis of their CRISPR repeat sequences. A few short 2 - 5 bp sequences were identified adjacent to one end of the protospacers. Experimental and bioinformatical results linked the motif to the excision of protospacers and their insertion into CRISPR loci. Subsequently, evidence accumulated from different virus- and plasmid-targeting assays, suggesting that these motifs were also recognized during DNA interference, at least for the recently classified type I and type II CRISPR-based systems. The two processes, spacer acquisition and protospacer interference, employ different molecular mechanisms, and there is increasing evidence to suggest that the sequence motifs that are recognized, while overlapping, are unlikely to be identical. In this article,we consider the properties of PAM sequences and summarize the evidence for their dual functional roles. It is proposed to use the terms protospacer associated motif (PAM) for the conserved DNA sequence and to employ spacer acqusition motif (SAM) and target interference motif (TIM), respectively, for acquisition and interference recognition sites.
机译:Protospacer相邻基序(PAM)最初是针对CRISPR-Cas系统进行表征的,该系统根据其CRISPR重复序列进行分类。在原间隔子的一端附近鉴定出一些短的2-5 bp序列。实验和生物信息学结果将该基序与原间隔子的切除及其插入CRISPR基因座相关联。随后,从不同的针对病毒和质粒的靶向分析中收集到的证据表明,至少在最近分类的基于I型和II型CRISPR的系统中,这些基序也被DNA干扰识别。间隔物获取和原间隔物干扰这两个过程采用不同的分子机制,并且越来越多的证据表明,虽然重叠,但被识别的序列基序不可能相同。在本文中,我们考虑了PAM序列的特性,并总结了其双重功能的证据。建议将术语原间隔子相关基序(PAM)用于保守的DNA序列,并分别将间隔捕获基序(SAM)和靶干扰基序(TIM)用于捕获和干扰识别位点。

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