Mannose Antagonizes GSDME-mediated Pyroptosis Through AMPK Activated by Metabolite GlcNAc-6P

Overview

Journal Cell Res

Specialty Cell Biology

Date 2023 Jul 17

PMID 37460805

Authors

Yuan-Li Ai

Wei-Jia Wang

Fan-Jian Liu

Wei Fang

Hang-Zi Chen

Liu-Zheng Wu

Xuehui Hong

Yuekun Zhu

Ci-Xiong Zhang

Long-Yu Liu

Wen-Bin Hong

Bo Zhou

Qi-Tao Chen

Qiao Wu

Affiliations

Soon will be listed here.

Abstract

Pyroptosis is a type of regulated cell death executed by gasdermin family members. However, how gasdermin-mediated pyroptosis is negatively regulated remains unclear. Here, we demonstrate that mannose, a hexose, inhibits GSDME-mediated pyroptosis by activating AMP-activated protein kinase (AMPK). Mechanistically, mannose metabolism in the hexosamine biosynthetic pathway increases levels of the metabolite N-acetylglucosamine-6-phosphate (GlcNAc-6P), which binds AMPK to facilitate AMPK phosphorylation by LKB1. Activated AMPK then phosphorylates GSDME at Thr6, which leads to blockade of caspase-3-induced GSDME cleavage, thereby repressing pyroptosis. The regulatory role of AMPK-mediated GSDME phosphorylation was further confirmed in AMPK knockout and GSDME or GSDME knock-in mice. In mouse primary cancer models, mannose administration suppressed pyroptosis in small intestine and kidney to alleviate cisplatin- or oxaliplatin-induced tissue toxicity without impairing antitumor effects. The protective effect of mannose was also verified in a small group of patients with gastrointestinal cancer who received normal chemotherapy. Our study reveals a novel mechanism whereby mannose antagonizes GSDME-mediated pyroptosis through GlcNAc-6P-mediated activation of AMPK, and suggests the utility of mannose supplementation in alleviating chemotherapy-induced side effects in clinic applications.

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