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Heavily Armed Ancestors: CRISPR Immunity and Applications in Archaea with a Comparative Analysis of CRISPR Types in Sulfolobales

机译:严重武装的祖先:Archaea中的Crisprp免疫和应用,对亚磺醛碱的比较分析

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摘要

Prokaryotes are constantly coping with attacks by viruses in their natural environments and therefore have evolved an impressive array of defense systems. Clustered Regularly Interspaced Short Palindromic Repeats (CRISPR) is an adaptive immune system found in the majority of archaea and about half of bacteria which stores pieces of infecting viral DNA as spacers in genomic CRISPR arrays to reuse them for specific virus destruction upon a second wave of infection. In detail, small CRISPR RNAs (crRNAs) are transcribed from CRISPR arrays and incorporated into type-specific CRISPR effector complexes which further degrade foreign nucleic acids complementary to the crRNA. This review gives an overview of CRISPR immunity to newcomers in the field and an update on CRISPR literature in archaea by comparing the functional mechanisms and abundances of the diverse CRISPR types. A bigger fraction is dedicated to the versatile and prevalent CRISPR type III systems, as tremendous progress has been made recently using archaeal models in discerning the controlled molecular mechanisms of their unique tripartite mode of action including RNA interference, DNA interference and the unique cyclic-oligoadenylate signaling that induces promiscuous RNA shredding by CARF-domain ribonucleases. The second half of the review spotlights CRISPR in archaea outlining seminal in vivo and in vitro studies in model organisms of the euryarchaeal and crenarchaeal phyla, including the application of CRISPR-Cas for genome editing and gene silencing. In the last section, a special focus is laid on members of the crenarchaeal hyperthermophilic order Sulfolobales by presenting a thorough comparative analysis about the distribution and abundance of CRISPR-Cas systems, including arrays and spacers as well as CRISPR-accessory proteins in all 53 genomes available to date. Interestingly, we find that CRISPR type III and the DNA-degrading CRISPR type I complexes co-exist in more than two thirds of these genomes. Furthermore, we identified ring nuclease candidates in all but two genomes and found that they generally co-exist with the above-mentioned CARF domain ribonucleases Csx1/Csm6. These observations, together with published literature allowed us to draft a working model of how CRISPR-Cas systems and accessory proteins cross talk to establish native CRISPR anti-virus immunity in a Sulfolobales cell.
机译:原核生在自然环境中,病毒不断应对攻击,因此已经发展了令人印象深刻的一系列防御系统。聚集在一起的短文重复(CRISPR)是一种自适应免疫系统,其在大多数古痤疮和大约一半的细菌中,它将感染病毒DNA的碎片作为基因组CRISPR阵列中的间隔物,以重复使用它们在第二波上的特定病毒破坏感染。详细地,小的CRISPR RNA(CRRNA)从CRISPR阵列转录并掺入特定类型的CRISPR效应复合物中,其进一步降解与CRRNA互补的外核酸。本综述概述了通过比较各种CRISPR类型的功能机制和丰富的功能机制和丰富,概述了该领域的新人和古代克里普尔文学的更新。更大的分数是致力于多功能和普遍的CRISPR型III系统,因为最近使用古代模型在辨别出其独特的三方作用模式的受控分子机制中的巨大进展,包括RNA干扰,DNA干扰和独特的环寡烯酸通过CARF结构域核糖核酸酶诱导混杂RNA粉碎的信号传导。下半年审查聚光灯在古代体内概述初创性和体外研究的euryarchaeal和颅骨的模型生物体中的体外研究,包括用于基因组编辑和基因沉默的CRISPR-CAS的应用。在最后一节中,通过呈现关于CRISPR-CAS系统的分布和丰度的彻底的比较分析,包括阵列和垫片以及所有53种基因组中的阵列和垫片的彻底比较分析可使用迄今为止。有趣的是,我们发现CRISPR型III和DNA降级CRISPR型I复合物共存在这些基因组的超过三分之二。此外,我们在所有两个基因组中鉴定了环核酸酶候选者,发现它们通常与上述CARF结构核核酸酶CSX1 / CSM6共存。这些观察结果与发表的文献一起使我们能够起草如何在Cris-Cas系统和附件蛋白质交叉谈话中如何在亚磺脲类细胞中建立天然克里普尔抗病毒免疫力的工作模型。

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