ROS-dependent S-palmitoylation Activates Cleaved and Intact Gasdermin D

Overview

Journal Nature

Specialty Science

Date 2024 Apr 10

PMID 38599239

Authors

Gang Du

Liam B Healy

Liron David

Caitlin Walker

Tarick J El-Baba

Corinne A Lutomski

Byoungsook Goh

Bowen Gu

Xiong Pi

Pascal Devant

Pietro Fontana

Ying Dong

Xiyu Ma

Rui Miao

Arumugam Balasubramanian

Robbins Puthenveetil

Anirban Banerjee

Hongbo R Luo

Jonathan C Kagan

Sungwhan F Oh

Carol V Robinson

Judy Lieberman

Hao Wu

Affiliations

Soon will be listed here.

Abstract

Gasdermin D (GSDMD) is the common effector for cytokine secretion and pyroptosis downstream of inflammasome activation and was previously shown to form large transmembrane pores after cleavage by inflammatory caspases to generate the GSDMD N-terminal domain (GSDMD-NT). Here we report that GSDMD Cys191 is S-palmitoylated and that palmitoylation is required for pore formation. S-palmitoylation, which does not affect GSDMD cleavage, is augmented by mitochondria-generated reactive oxygen species (ROS). Cleavage-deficient GSDMD (D275A) is also palmitoylated after inflammasome stimulation or treatment with ROS activators and causes pyroptosis, although less efficiently than palmitoylated GSDMD-NT. Palmitoylated, but not unpalmitoylated, full-length GSDMD induces liposome leakage and forms a pore similar in structure to GSDMD-NT pores shown by cryogenic electron microscopy. ZDHHC5 and ZDHHC9 are the major palmitoyltransferases that mediate GSDMD palmitoylation, and their expression is upregulated by inflammasome activation and ROS. The other human gasdermins are also palmitoylated at their N termini. These data challenge the concept that cleavage is the only trigger for GSDMD activation. They suggest that reversible palmitoylation is a checkpoint for pore formation by both GSDMD-NT and intact GSDMD that functions as a general switch for the activation of this pore-forming family.

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