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新型噬菌体衍生抗菌酶 PolaR 靶向 spp.

New Phage-Derived Antibacterial Enzyme PolaR Targeting spp.

机构信息

Hirszfeld Institute of Immunology and Experimental Therapy, Polish Academy of Sciences, 53-114 Wrocław, Poland.

Department of Molecular Virology, Faculty of Biology, Adam Mickiewicz University, 61-712 Poznań, Poland.

出版信息

Cells. 2023 Aug 4;12(15):1997. doi: 10.3390/cells12151997.

Abstract

is an opportunistic pathogen, particularly life-threatening for the immunocompromised. It is associated with pneumonia, endocarditis, peritonitis and many other serious infections, including septicemia. Of note, produces metabolites that support and increase overgrowth of , one of the ESKAPE bacteria. Endolysins are considered as antibacterial enzymes derived from bacteriophages that selectively and efficiently kill susceptible bacteria without harming human cells or the normal microbiome. Here, we applied a computational analysis of metagenomic sequencing data of the gastric mucosa phageome extracted from human patients' stomach biopsies. A selected candidate anti- sequence was produced in an expression system, purified and confirmed as a - and -specific endolysin PolaR, able to destroy bacterial cells even when aggregated, as in a biofilm. PolaR had no cytotoxic or antiproliferative effects on mammalian cells. PolaR is the first described endolysin selectively targeting species, with a high potential to combat infections caused by and , and possibly other bacterial groups. PolaR is the first antibacterial enzyme selected from the gastric mucosa phageome, which underlines the biological complexity and probably underestimated biological role of the phageome in the human gastric mucosa.

摘要

是一种机会性病原体,对免疫功能低下者尤其具有致命性。它与肺炎、心内膜炎、腹膜炎和许多其他严重感染有关,包括败血症。值得注意的是,产生的代谢物支持和增加 的过度生长, 是 ESKAPE 细菌之一。内溶素被认为是来源于噬菌体的抗菌酶,它们能够选择性和有效地杀死易感细菌,而不会伤害人类细胞或正常微生物组。在这里,我们应用了对从人类胃活检中提取的胃黏膜噬菌体组的宏基因组测序数据的计算分析。从表达系统中产生了一个选定的候选抗 序列,经过纯化并确认为 和 特异性内溶素 PolaR,能够破坏即使聚集在一起的细菌细胞,如生物膜。PolaR 对哺乳动物细胞没有细胞毒性或抗增殖作用。PolaR 是第一个被描述的选择性针对 物种的内溶素,具有很高的潜力来对抗由 和 引起的感染,可能还有其他细菌群。PolaR 是从胃黏膜噬菌体组中选择的第一个抗菌酶,这突显了噬菌体组在人类胃黏膜中的生物学复杂性和可能被低估的生物学作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b02/10417112/8f33c14a8117/cells-12-01997-g001.jpg

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