| Literature DB >> 35110732 |
Wanyan Deng1,2,3, Yang Bai1,4, Fan Deng1,4, Youdong Pan5,6, Shenglin Mei7, Zengzhang Zheng1,2,3, Rui Min1,4, Zeyu Wu1,4, Wu Li1,2,3, Rui Miao8,9, Zhibin Zhang8,9, Thomas S Kupper5,6, Judy Lieberman8,9, Xing Liu10,11,12.
Abstract
Gasdermins, a family of five pore-forming proteins (GSDMA-GSDME) in humans expressed predominantly in the skin, mucosa and immune sentinel cells, are key executioners of inflammatory cell death (pyroptosis), which recruits immune cells to infection sites and promotes protective immunity1,2. Pore formation is triggered by gasdermin cleavage1,2. Although the proteases that activate GSDMB, C, D and E have been identified, how GSDMA-the dominant gasdermin in the skin-is activated, remains unknown. Streptococcus pyogenes, also known as group A Streptococcus (GAS), is a major skin pathogen that causes substantial morbidity and mortality worldwide3. Here we show that the GAS cysteine protease SpeB virulence factor triggers keratinocyte pyroptosis by cleaving GSDMA after Gln246, unleashing an active N-terminal fragment that triggers pyroptosis. Gsdma1 genetic deficiency blunts mouse immune responses to GAS, resulting in uncontrolled bacterial dissemination and death. GSDMA acts as both a sensor and substrate of GAS SpeB and as an effector to trigger pyroptosis, adding a simple one-molecule mechanism for host recognition and control of virulence of a dangerous microbial pathogen.Entities:
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Year: 2022 PMID: 35110732 DOI: 10.1038/s41586-021-04384-4
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 69.504