Group 2 innate lymphoid cells constrain type 3/17 lymphocytes in shared stromal niches to restrict liver fibrosis

Author:

Sbierski-Kind Julia,Cautivo Kelly M,Wagner Johanna C,Dahlgren Madelene W,Nilsson Julia,Krasilnikov Maria,Mroz Nicholas M.,Lizama Carlos O.,Gan Anna Lu,Matatia Peri R,Taruselli Marcela T,Chang Anthony A,Caryotakis Sofia,O’Leary Claire E,Kotas Maya,Mattis Aras NORCID,Peng Tien,Locksley Richard M,Molofsky Ari B

Abstract

SUMMARYGroup 2 innate lymphoid cells (ILC2s) cooperate with adaptive Th2 cells as key organizers of tissue type 2 immune responses, while a spectrum of innate and adaptive lymphocytes coordinate early type 3/17 immunity. Both type 2 and type 3/17 lymphocyte associated cytokines are linked to tissue fibrosis, but how their dynamic and spatial topographies may direct beneficial or pathologic organ remodelling is unclear. Here we used volumetric imaging in models of liver fibrosis, finding accumulation of periportal and fibrotic tract IL-5+lymphocytes, predominantly ILC2s, in close proximity to expanded type 3/17 lymphocytes and IL-33highniche fibroblasts. Ablation of IL-5+lymphocytes worsened carbon tetrachloride-and bile duct ligation-induced liver fibrosis with increased niche IL-17A+type 3/17 lymphocytes, predominantly γδ T cells. In contrast, concurrent ablation of IL-5+and IL-17A+lymphocytes reduced this progressive liver fibrosis, suggesting a cross-regulation of type 2 and type 3 lymphocytes at specialized fibroblast niches that tunes hepatic fibrosis.

Publisher

Cold Spring Harbor Laboratory

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