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首页> 外文期刊>Journal of Molecular Biology >Tuning in to interference: R-loops and cascade complexes in CRISPR immunity
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Tuning in to interference: R-loops and cascade complexes in CRISPR immunity

机译:调整干扰:CRISPR免疫中的R环和级联复合物

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Stable RNA-DNA hybrids formed by invasion of an RNA strand into duplex DNA, termed R-loops, are notorious for provoking genome instability especially when they arise during transcription. However, in some instances (DNA replication and class switch recombination), R-loops are useful so long as their existence is carefully managed to avoid them persisting. A recent flow of research papers establishes a newly discovered use for R-loops as key intermediates in a prokaryotic immune system called CRISPR (Clustered Regularly Interspersed Short Palindromic Repeats). Structures and mechanism of ribonucleoprotein complexes (Cascades) that form CRISPR R-loops highlight precision targeting of duplex DNA that has sequence characteristics marking it as foe, enabling nucleolytic destruction of DNA and recycling the Cascade. We review these significant recent breakthroughs in understanding targeting/interference stages of CRISPR immunity and discuss questions arising, including a possible link between targeting and adaptive immunity in prokaryotes.
机译:通过将RNA链侵入双链体DNA形成的稳定的RNA-DNA杂合体(称为R环),会引起基因组不稳定,尤其是在转录过程中出现时,这是众所周知的。但是,在某些情况下(DNA复制和类开关重组),R环是有用的,只要仔细管理它们的存在以避免它们持久存在即可。最近的研究论文流为R环建立了新发现的用途,将其作为称为CRISPR(成簇规则散布的短回文重复序列)的原核免疫系统的关键中间体。形成CRISPR R环的核糖核蛋白复合物(Cascades)的结构和机制突出了对双链DNA的精确靶向,该序列具有将其标记为敌人的序列特征,从而能够进行核酸的核酸破坏并回收Cascade。我们回顾了这些最近在理解CRISPR免疫的靶向/干扰阶段方面的重大突破,并讨论了出现的问题,包括原核生物中靶向与适应性免疫之间的可能联系。

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