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Strong bias in the bacterial CRISPR elements that confer immunity to phage

机译:赋予细菌对噬菌体免疫力的细菌CRISPR元件产生强烈偏见

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Clustered regularly interspaced short palindromic repeats (CRISPR)–Cas systems provide adaptive immunity against phage via spacer-encoded CRISPR RNAs that are complementary to invasive nucleic acids. Here, we challenge Streptococcus thermophilus with a bacteriophage, and used PCR-based metagenomics to monitor phage-derived spacers daily for 15 days in two experiments. Spacers that target the host chromosome are infrequent and strongly selected against, suggesting autoimmunity is lethal. In experiments that recover over half a million spacers, we observe early dominance by a few spacer sub-populations and rapid oscillations in sub-population abundances. In two CRISPR systems and in replicate experiments, a few spacers account for the majority of spacer sequences. Nearly all phage locations targeted by the acquired spacers have a proto-spacer adjacent motif (PAM), indicating PAMs are involved in spacer acquisition. We detect a strong and reproducible bias in the phage genome locations from which spacers derive. This may reflect selection for specific spacers based on location and effectiveness.
机译:簇状规则间隔的短回文重复序列(CRISPR)-Cas系统通过与侵入性核酸互补的间隔子编码CRISPR RNA提供针对噬菌体的适应性免疫。在这里,我们用噬菌体挑战嗜热链球菌,并在两个实验中每天使用基于PCR的宏基因组学来监测噬菌体衍生的间隔子,持续15天。靶向宿主染色体的间隔子很少见,强烈选择反对,表明自身免疫是致命的。在回收了超过一百万个间隔子的实验中,我们观察到了一些间隔子亚群的早期优势,以及子群丰度的快速振荡。在两个CRISPR系统和重复实验中,少数间隔区占了大部分间隔区序列。所获得的间隔子靶向的几乎所有噬菌体位置均具有原间隔子邻近基序(PAM),表明PAM参与了间隔子的获取。我们检测到间隔物从其衍生的噬菌体基因组位置中的强大和可重现的偏见。这可以反映出基于位置和有效性对特定间隔物的选择。

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