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RNA Targeting by the Type III-A CRISPR-Cas Csm Complex of Thermus thermophilus

机译:嗜热栖热菌III-A型CRISPR-Cas Csm复合体的RNA靶向

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摘要

CRISPR-Cas is a prokaryotic adaptive immune system that provides sequence-specific defense against foreign nucleic acids. Here we report the structure and function of the effector complex of the Type III-A CRISPR-Cas system of Thermus thermophilus: the Csm complex (TtCsm). TtCsm is composed of five different protein subunits (Csm1-Csm5) with an uneven stoichiometry and a single crRNA of variable size (35-53 nt). The TtCsm crRNA content is similar to the Type III-B Cmr complex, indicating that crRNAs are shared among different subtypes. A negative stain EM structure of the TtCsm complex exhibits the characteristic architecture of Type I and Type III CRISPR-associated ribonucleoprotein complexes. crRNA-protein crosslinking studies show extensive contacts between the Csm3 backbone and the bound crRNA. We show that, like TtCmr, TtCsm cleaves complementary target RNAs at multiple sites. Unlike Type I complexes, interference by TtCsm does not proceed via initial base pairing by a seed sequence.
机译:CRISPR-Cas是一种原核适应性免疫系统,可提供针对外来核酸的序列特异性防御​​。在这里,我们报告嗜热栖热菌的III-A型CRISPR-Cas系统效应复合物的结构和功能:Csm复合物(TtCsm)。 TtCsm由五个不同的蛋白亚基(Csm1-Csm5)组成,它们的化学计量不均,并且单个crRNA的大小不一(35-53 nt)。 TtCsm crRNA含量与III-B型Cmr复合体相似,表明crRNA在不同亚型之间共享。 TtCsm复合物的负染色EM结构表现出I型和III型CRISPR相关核糖核蛋白复合物的特征结构。 crRNA-蛋白质交联研究表明Csm3主链与结合的crRNA之间广泛接触。我们显示,像TtCmr一样,TtCsm在多个位点切割互补的靶RNA。与I型复合物不同,TtCsm的干扰不会通过种子序列的初始碱基配对进行。

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