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乳品噬菌体通过抗 CRISPR 蛋白 AcrIIA3 逃避嗜热链球菌的 CRISPR 防御。

Dairy phages escape CRISPR defence of Streptococcus thermophilus via the anti-CRISPR AcrIIA3.

机构信息

Département de biochimie, de microbiologie, et de bio-informatique, Faculté des sciences et de génie, Université Laval, Québec, QC, Canada; Groupe de recherche en écologie buccale, Faculté de médecine dentaire, Université Laval, Québec, QC, Canada.

Département de biochimie, de microbiologie, et de bio-informatique, Faculté des sciences et de génie, Université Laval, Québec, QC, Canada; Groupe de recherche en écologie buccale, Faculté de médecine dentaire, Université Laval, Québec, QC, Canada; Department of Fundamental Microbiology, University of Lausanne, Lausanne, Switzerland; Agroscope, Bern, Switzerland.

出版信息

Int J Food Microbiol. 2023 Dec 16;407:110414. doi: 10.1016/j.ijfoodmicro.2023.110414. Epub 2023 Sep 22.

Abstract

Bacterial community collapse due to phage infection is a major risk in cheese making processes. As virulent phages are ubiquitous and diverse in milk fermentation factories, the use of phage-resistant lactic acid bacteria (LAB) is essential to obtain high-quality fermented dairy products. The LAB species Streptococcus thermophilus contains two type II-A CRISPR-Cas systems (CRISPR1 and CRISPR3) that can effectively protect against phage infection. However, virulent streptococcal phages carrying anti-CRISPR proteins (ACR) that block the activity of CRISPR-Cas systems have emerged in yogurt and cheese environments. For example, phages carrying AcrIIA5 can impede both CRISPR1 and CRISPR3 systems, while AcrIIA6 stops only CRISPR1. Here, we explore the activity and diversity of a third streptococcal phage anti-CRISPR protein, namely AcrIIA3. We were able to demonstrate that AcrIIA3 is efficiently active against the CRISPR3-Cas system of S. thermophilus. We used AlphaFold2 to infer the structure of AcrIIA3 and we predicted that this new family of functional ACR in virulent streptococcal phages has a new α-helical fold, with no previously identified structural homologs. Because ACR proteins are being explored as modulators in genome editing applications, we also tested AcrIIA3 against SpCas9. We found that AcrIIA3 could block SpCas9 in bacteria but not in human cells. Understanding the diversity and functioning of anti-defence mechanisms will be of importance in the design of long-term stable starter cultures.

摘要

噬菌体感染导致的细菌群落崩溃是奶酪制作过程中的主要风险。由于烈性噬菌体在牛奶发酵工厂中无处不在且种类繁多,因此使用抗噬菌体的乳酸菌(LAB)对于获得高质量的发酵乳制品至关重要。LAB 物种嗜热链球菌包含两个 II-A 型 CRISPR-Cas 系统(CRISPR1 和 CRISPR3),可以有效抵御噬菌体感染。然而,在酸奶和奶酪环境中,出现了携带抗 CRISPR 蛋白(ACR)的烈性链球菌噬菌体,这些 ACR 可以阻断 CRISPR-Cas 系统的活性。例如,携带 AcrIIA5 的噬菌体可以阻止 CRISPR1 和 CRISPR3 系统的活性,而 AcrIIA6 仅阻止 CRISPR1 系统的活性。在这里,我们研究了第三种链球菌噬菌体抗 CRISPR 蛋白,即 AcrIIA3 的活性和多样性。我们能够证明 AcrIIA3 可以有效地针对嗜热链球菌的 CRISPR3-Cas 系统发挥作用。我们使用 AlphaFold2 推断 AcrIIA3 的结构,并预测这种新的功能 ACR 在烈性链球菌噬菌体中的家族具有新的α-螺旋折叠,没有以前确定的结构同源物。由于 ACR 蛋白被探索作为基因组编辑应用中的调节剂,我们还针对 SpCas9 测试了 AcrIIA3。我们发现 AcrIIA3 可以在细菌中阻断 SpCas9,但不能在人类细胞中阻断。了解抗防御机制的多样性和功能对于设计长期稳定的起始培养物将非常重要。

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