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Spacer acquisition by Type III CRISPR–Cas system during bacteriophage infection of Thermus thermophilus

机译:Spacer通过III型CRISPR-CAS系统在噬菌体感染过程中的热嗜热杆菌

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Type III CRISPR–Cas systems provide immunity to foreign DNA by targeting its transcripts. Target recognition activates RNases and DNases that may either destroy foreign DNA directly or elicit collateral damage inducing death of infected cells. While some Type III systems encode a reverse transcriptase to acquire spacers from foreign transcripts, most contain conventional spacer acquisition machinery found in DNA-targeting systems. We studied Type III spacer acquisition in phage-infected Thermus thermophilus, a bacterium that lacks either a standalone reverse transcriptase or its fusion to spacer integrase Cas1. Cells with spacers targeting a subset of phage transcripts survived the infection, indicating that Type III immunity does not operate through altruistic suicide. In the absence of selection spacers were acquired from both strands of phage DNA, indicating that no mechanism ensuring acquisition of RNA-targeting spacers exists. Spacers that protect the host from the phage demonstrate a very strong strand bias due to positive selection during infection. Phages that escaped Type III interference accumulated deletions of integral number of codons in an essential gene and much longer deletions in a non-essential gene. This and the fact that Type III immunity can be provided by plasmid-borne mini-arrays open ways for genomic manipulation of Thermus phages.
机译:III型CRISPR-CAS系统通过靶向其转录物来为外国DNA提供免疫力。目标识别激活rNases和dNases,其可以直接破坏外国DNA或引发诱导感染细胞死亡的抵押损伤。虽然某些III型系统编码逆转录酶以获取来自外部转录物的间隔物,但大多数含有在DNA靶向系统中发现的常规间隔采集机制。我们在噬菌体感染的热嗜热杆菌中研究了III型间隔采集,一种缺乏独立逆转录酶的细菌或其融合到间隔整合酶Cas1。靶向噬菌体转录物子集的间隔物的细胞存活了感染,表明III型免疫不能通过利他制法。在没有选择间隔物的情况下,从两条噬菌体DNA中获得,表明不存在确保采集RNA靶向间隔物的机制。保护宿主免受噬菌体的垫片表明,由于感染期间的阳性选择,呈现出非常强烈的链偏差。跳过III型干扰的噬菌体在非必需基因中累积III型干扰积累缺失基因组中积分数量的密码子的缺失。这是III型免疫的事实可以通过质粒 - 传播的迷你阵列提供用于热噬菌体的基因组操纵方法。

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