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Spacer Acquisition Rates Determine the Immunological Diversity of the Type II CRISPR-Cas Immune Response

机译:间隔采集率确定II型CRISPR-CAS免疫反应的免疫多样性

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CRISPR-Cas systems provide acquired immunity in prokaryotes. Upon infection, short sequences from the phage genome, known as spacers, are inserted between the CRISPR repeats. Spacers are transcribed into small RNA molecules that guide nucleases to their targets. The forces that shape the distribution of newly acquired spacers, which is observed to be uneven, are poorly understood. We studied the spacer patterns that arise after phage infection of Staphylococcus aureus harboring the Streptococcus pyogenes type II-A CRISPR-Cas system. We observed that spacer patterns are established early during the CRISPR-Cas immune response and correlate with spacer acquisition rates, but not with spacer targeting efficiency. The rate of spacer acquisition depended on sequence elements within the spacer, which in turn determined the abundance of different spacers within the adapted population. Our results reveal how the two main forces of the CRISPR-Cas immune response, acquisition and targeting, affect the generation of immunological diversity.
机译:CRISPR-CAS系统在原核生物中提供了患有的免疫力。在感染时,从噬菌体基因组中的短序列被称为垫片,在CRISPR重复之间插入。垫片被转录成小RNA分子,以指导核酸酶到其靶标。塑造了新获得的间隔物的分布的力,观察到不均匀,理解得不景气。我们研究了在含有II型-A CRISPR-CAS系统的链球菌化脓性的金黄色葡萄球菌的噬菌体感染后出现的间隔模式。我们观察到,间隔模式是在CRIS-CAS免疫应答期间提前建立的,与间隔采集率相关,但不具有间隔率靶向效率。间隔率采集率依赖于间隔件内的序列元件,其又确定了适应群体内的不同间隔物的丰度。我们的结果揭示了CRISPR-CAS免疫反应,收购和靶向的两个主要力量如何影响免疫多样性的产生。

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