Up-regulation of Gasdermin C in Mouse Small Intestine is Associated with Lytic Cell Death in Enterocytes in Worm-induced Type 2 Immunity

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2021 Jul 22

PMID 34290141

Citations 30

Authors

Ranhui Xi

Julia Montague

Xiaoli Lin

Chanyi Lu

Weiwei Lei

Keisuke Tanaka

Yali V Zhang

Xin Xu

Xin Zheng

Xuedong Zhou

Joseph F Urban Jr

Ken Iwatsuki

Robert F Margolskee

Ichiro Matsumoto

Marco Tizzano

Jiyao Li

Peihua Jiang

Affiliations

Soon will be listed here.

Abstract

"Taste-like" tuft cells in the intestine trigger type 2 immunity in response to worm infection. The secretion of interleukin-13 (IL-13) from type 2 innate lymphoid cells (ILC2) represents a key step in the tuft cell-ILC2 cell-intestinal epithelial cell circuit that drives the clearance of worms from the gut via type 2 immune responses. Hallmark features of type 2 responses include tissue remodeling, such as tuft and goblet cell expansion, and villus atrophy, yet it remains unclear if additional molecular changes in the gut epithelium facilitate the clearance of worms from the gut. Using gut organoids, we demonstrated that IL-4 and IL-13, two type 2 cytokines with similar functions, not only induced the classical type 2 responses (e.g., tuft cell expansion) but also drastically up-regulated the expression of gasdermin C genes (s). Using an in vivo worm-induced type 2 immunity model, we confirmed the up-regulation of s in -infected wild-type C57BL/6 mice. Consistent with gasdermin family members being principal effectors of pyroptosis, overexpression of Gsdmc2 in human embryonic kidney 293 (HEK293) cells triggered pyroptosis and lytic cell death. Moreover, in intestinal organoids treated with IL-4 or IL-13, or in wild-type mice infected with , lytic cell death increased, which may account for villus atrophy observed in worm-infected mice. Thus, we propose that the up-regulated Gsdmc family may be major effectors for type 2 responses in the gut and that Gsdmc-mediated pyroptosis may provide a conduit for the release of antiparasitic factors from enterocytes to facilitate the clearance of worms.

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