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生物膜形成功能淀粉样蛋白 PSMα1 的结构来自.

Structure of biofilm-forming functional amyloid PSMα1 from .

机构信息

Department of Structural Biology, School of Medicine, University of Pittsburgh, Pittsburgh, PA 15261.

Department of Biomedicine, Aarhus University, Aarhus 8000, Denmark.

出版信息

Proc Natl Acad Sci U S A. 2024 Aug 13;121(33):e2406775121. doi: 10.1073/pnas.2406775121. Epub 2024 Aug 8.

Abstract

Biofilm-protected pathogenic causes chronic infections that are difficult to treat. An essential building block of these biofilms are functional amyloid fibrils that assemble from phenol-soluble modulins (PSMs). PSMα1 cross-seeds other PSMs into cross-β amyloid folds and is therefore a key element in initiating biofilm formation. However, the paucity of high-resolution structures hinders efforts to prevent amyloid assembly and biofilm formation. Here, we present a 3.5 Å resolution density map of the major PSMα1 fibril form revealing a left-handed cross-β fibril composed of two C-symmetric U-shaped protofilaments whose subunits are unusually tilted out-of-plane. Monomeric α-helical PSMα1 is extremely cytotoxic to cells, despite the moderate toxicity of the cross-β fibril. We suggest mechanistic insights into the PSM functional amyloid formation and conformation transformation on the path from monomer-to-fibril formation. Details of PSMα1 assembly and fibril polymorphism suggest how utilizes functional amyloids to form biofilms and establish a framework for developing therapeutics against infection and antimicrobial resistance.

摘要

生物膜保护的病原菌导致难以治疗的慢性感染。这些生物膜的基本组成部分是功能性淀粉样原纤维,它们由酚溶性调节蛋白(PSM)组装而成。PSMα1 将其他 PSM 交叉成交叉-β 淀粉样折叠,因此是启动生物膜形成的关键因素。然而,高分辨率结构的缺乏阻碍了防止淀粉样组装和生物膜形成的努力。在这里,我们展示了主要 PSMα1 纤维形式的 3.5 Å 分辨率密度图,揭示了由两个 C 对称 U 形原纤维组成的左手交叉-β 纤维,其亚基异常倾斜出平面。单体α-螺旋 PSMα1 对细胞具有极强的细胞毒性,尽管交叉-β 纤维的毒性适中。我们提出了关于 PSM 功能淀粉样形成的机制见解,并在单体到纤维形成的过程中构象转化。PSMα1 组装和纤维多态性的细节表明了 如何利用功能淀粉样蛋白形成生物膜,并为开发针对感染和抗微生物耐药性的治疗方法提供了框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3812/11331129/a3c85326ac7d/pnas.2406775121fig01.jpg

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