AI Article Synopsis

  • * The SPI-2 effector SseK3 inhibits the normal pairing of SNARE proteins, which are essential for vesicle fusion, leading to the formation of harmful filaments in infected cells.
  • * Host cells respond by activating the E3 ubiquitin ligase TRIM32, which targets SseK3 for degradation, thereby reducing its impact and inhibiting bacterial replication.

Article Abstract

Typhimurium creates an intracellular niche for its replication by utilizing a large cohort of effectors, including several that function to interfere with host ubiquitin signaling. Although the mechanism of action of many such effectors has been elucidated, how the interplay between the host ubiquitin network and bacterial virulence factors dictates the outcome of infection largely remains undefined. In this study, we found that the SPI-2 effector SseK3 inhibits SNARE pairing to promote the formation of a -induced filament by Arg-GlcNAcylation of SNARE proteins, including SNAP25, VAMP8, and Syntaxin. Further study reveals that host cells counteract the activity of SseK3 by inducing the expression of the E3 ubiquitin ligase TRIM32, which catalyzes K48-linked ubiquitination on SseK3 and targets its membrane-associated portion for degradation. Hence, TRIM32 antagonizes SNAP25 Arg-GlcNAcylation induced by SseK3 to restrict -induced filament biogenesis and replication. Our study reveals a mechanism by which host cells inhibit bacterial replication by eliminating specific virulence factors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10989757PMC
http://dx.doi.org/10.1002/mlf2.12063DOI Listing

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