Salmonella manipulates macrophage migration via SteC-mediated myosin light chain activation to penetrate the gut-vascular barrier

Author:

Dai YuanjiORCID,Zhang MinORCID,Liu XiaoyuORCID,Sun Ting,Qi Wenqi,Ding Wei,Chen ZheORCID,Zhang PingORCID,Liu Ruirui,Chen Huimin,Chen Siyan,Wang Yuzhen,Yue Yingying,Song Nannan,Wang Weiwei,Jia Haihong,Ma Zhongrui,Li Cuiling,Chen QixinORCID,Li BingqingORCID

Abstract

AbstractThe intestinal pathogen Salmonella enterica rapidly enters the bloodstream after the invasion of intestinal epithelial cells, but how Salmonella breaks through the gut-vascular barrier is largely unknown. Here, we report that Salmonella enters the bloodstream through intestinal CX3CR1+ macrophages during early infection. Mechanistically, Salmonella induces the migration/invasion properties of macrophages in a manner dependent on host cell actin and on the pathogen effector SteC. SteC recruits host myosin light chain protein Myl12a and phosphorylates its Ser19 and Thr20 residues. Myl12a phosphorylation results in actin rearrangement, and enhanced migration and invasion of macrophages. SteC is able to utilize a wide range of NTPs other than ATP to phosphorylate Myl12a. We further solved the crystal structure of SteC, which suggests an atypical dimerization-mediated catalytic mechanism. Finally, in vivo data show that SteC-mediated cytoskeleton manipulation is crucial for Salmonella breaching the gut vascular barrier and spreading to target organs.

Funder

MOST | National Natural Science Foundation of China

Taishan Scholar Project of Shandong Province

山东省科学技术厅 | Natural Science Foundation of Shandong Province

Academic promotion programme of Shandong First Medical University

Publisher

Springer Science and Business Media LLC

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