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Co-evolution within structured bacterial communities results in multiple expansion of CRISPR loci and enhanced immunity

机译:结构化细菌群落内的共同进化导致CRISPR基因座的多重扩增和增强的免疫力

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摘要

Type II CRISPR-Cas systems provide immunity against phages and plasmids that infect bacteria through the insertion of a short sequence from the invader’s genome, known as the ‘spacer’, into the CRISPR locus. Spacers are transcribed into guide RNAs that direct the Cas9 nuclease to its target on the invader. In liquid cultures, most bacteria acquire a single spacer. Multiple spacer integration is a rare event which significance for immunity is poorly understood. Here, we found that when phage infections occur on solid media, a high proportion of the surviving colonies display complex morphologies that contain cells with multiple spacers. This is the result of the viral-host co-evolution, in which the immunity provided by the initial acquired spacer is easily overcome by escaper phages. Our results reveal the versatility of CRISPR-Cas immunity, which can respond with both single or multiple spacer acquisition schemes to solve challenges presented by different environments.
机译:II型CRISPR-Cas系统通过将来自入侵者基因组的短序列(称为“间隔子”)插入CRISPR基因座,从而提供针对感染细菌的噬菌体和质粒的免疫力。间隔子被转录成指导RNA,引导RNA引导Cas9核酸酶到达入侵者的靶标。在液体培养中,大多数细菌获得单个间隔物。多个间隔子整合是罕见的事件,对于免疫的重要性了解甚少。在这里,我们发现当噬菌体感染发生在固体培养基上时,很大一部分存活的菌落显示出复杂的形态,其中包含带有多个间隔子的细胞。这是病毒-宿主共同进化的结果,其中最初获得的间隔子提供的免疫力容易被逃避噬菌体克服。我们的研究结果揭示了CRISPR-Cas免疫的多功能性,可以通过单个或多个间隔子捕获方案来应对,以解决不同环境带来的挑战。

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