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首页> 外文期刊>FEMS Microbiology Letters >Unexpected connections between type VI-B CRISPR-Cas systems, bacterial natural competence, ubiquitin signaling network and DNA modification through a distinct family of membrane proteins
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Unexpected connections between type VI-B CRISPR-Cas systems, bacterial natural competence, ubiquitin signaling network and DNA modification through a distinct family of membrane proteins

机译:VI-B型CASP-SYSTEMS,细菌自然能力,泛素信号通信网络和DNA改性之间的意外连接通过不同的膜蛋白质

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摘要

In addition to core Cas proteins, CRISPR-Cas loci often encode ancillary proteins that modulate the activity of the respective effectors in interference. Subtype VI-B1 CRISPR-Cas systems encode the Csx27 protein that down-regulates the activity of Cas13b when the type VI-B locus is expressed in Escherichia coli. We show that Csx27 belongs to an expansive family of proteins that contain four predicted transmembrane helices and are typically encoded in predicted operons with components of the bacterial natural transformation machinery, multidomain proteins that consist of components of the ubiquitin signaling system and proteins containing the ligand-binding WYL domain and a helix-turn-helix domain. The Csx27 family proteins are predicted to form membrane channels for ssDNA that might comprise the core of a putative novel, Ub-regulated system for DNA uptake and, possibly, degradation. In addition to these associations, a distinct subfamily of the Csx27 family appears to be a part of a novel, membrane-associated system for DNA modification. In Bacteroidetes, subtype VI-B1 systems might degrade nascent transcripts of foreign DNA in conjunction with its uptake by the bacterial cell. These predictions suggest several experimental directions for the study of type VI CRISPR-Cas systems and distinct mechanisms of foreign DNA uptake and degradation in bacteria.
机译:除了核心CAS蛋白外,CRISPR-CAS基因座通常编码辅助蛋白,该蛋白质调节各种效应器的干扰活动。亚型VI-B1 CRISPR-CAS系统编码CSX27蛋白,当在大肠杆菌中表达VI-B座位点时,下调CAS13B的活性。我们表明CSX27属于含有四个预测的跨膜螺旋的膨胀蛋白质系列,并且通常在预测的操纵子中编码细菌天然转化机制的组分,多域蛋白质组成的多畴信号传导系统和含有配体的蛋白质的组分。绑定Wyl域和螺旋转螺旋域。预计CSX27系列蛋白质以形成用于SSDNA的膜通道,其可包括推定的新型UB调节系统的核心,用于DNA摄取,可能是降解。除了这些关联之外,CSX27家族的不同亚家族似乎是用于DNA改性的新型膜相关系统的一部分。在Bacteroidets中,亚型VI-B1系统可能与细菌细胞结合其摄取结合其产生的外来DNA的新生转录物。这些预测提出了若干实验方向,用于研究VI型CRAP-Systems,以及细菌中的外国DNA摄取和降解的不同机制。

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