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一种保守的噬菌体磷酸二酯酶能够逃避细菌的抗病毒免疫。

A conserved phage phosphoesterase enables evasion of bacterial antiviral immunity.

作者信息

Li Junlong, Song Yihao, Guo Xiao, He Zheng-Guo

机构信息

College of Life Science and Technology, Guangxi University, Nanning, 530004, China.

State Key Laboratory of Virology, Taikang Center for Life and Medical Sciences, TaiKang Medical School (School of Basic Medical Sciences), Wuhan University, Wuhan, 430071, China.

出版信息

EMBO Rep. 2025 May 29. doi: 10.1038/s44319-025-00488-4.

Abstract

With the increasing prevalence of drug-resistant bacteria, antimicrobial resistance emerges as a global public health threat. Mycobacteriophages show exciting prospects for the treatment of drug-resistant bacterial infections. However, the molecular mechanism through which they escape host bacterial defenses remains unclear. Here, we report that the gene gp48 of the mycobacteriophage A10ZJ24, which encodes a metallophosphoesterase-like protein, is essential for killing Mycobacterium tuberculosis. Gp48 is expressed during early stages of phage infection, and the Gp48 protein efficiently disrupts mycobacterial genomic DNA integrity, thereby silencing the expression of multiple anti-phage defense genes. While gp48-deletion phages infect and inject their DNA normally into M. tuberculosis cells, they are not able to impair the activation of the bacterial anti-phage genes which inhibit the replication of the genomic DNA of the mutant phage. This study thus identifies a phage metallophosphoesterase as a novel tool for subverting host bacterial antiviral immunity and killing M. tuberculosis. Our work fills a critical gap in the current knowledge on the arms race between mycobacteriophages and M. tuberculosis.

摘要

随着耐药菌的日益流行,抗菌药物耐药性已成为全球公共卫生威胁。分枝杆菌噬菌体在治疗耐药菌感染方面展现出令人兴奋的前景。然而,它们逃避宿主细菌防御的分子机制仍不清楚。在此,我们报告分枝杆菌噬菌体A10ZJ24的基因gp48编码一种类金属磷酸酯酶蛋白,对杀死结核分枝杆菌至关重要。Gp48在噬菌体感染的早期阶段表达,并且Gp48蛋白有效破坏分枝杆菌基因组DNA的完整性,从而使多个抗噬菌体防御基因的表达沉默。虽然缺失gp48的噬菌体能够正常感染并将其DNA注入结核分枝杆菌细胞,但它们无法削弱抑制突变噬菌体基因组DNA复制的细菌抗噬菌体基因的激活。因此,本研究确定了一种噬菌体金属磷酸酯酶是颠覆宿主细菌抗病毒免疫和杀死结核分枝杆菌的新工具。我们的工作填补了目前关于分枝杆菌噬菌体与结核分枝杆菌之间军备竞赛知识的关键空白。

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