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Mucus sialylation determines intestinal host-commensal homeostasis.

Authors :: Yao Y
Kim G
Shafer S
Chen Z
Kubo S
Ji Y
Luo J
Yang W
Perner SP
Kanellopoulou C
Park AY
Jiang P
Li J
Baris S
Aydiner EK
Ertem D
Mulder DJ
Warner N
Griffiths AM
Topf-Olivestone C
Kori M
Werner L
Ouahed J
Field M
Liu C
Schwarz B
Bosio CM
Ganesan S
Song J
Urlaub H
Oellerich T
Malaker SA
Zheng L
Bertozzi CR
Zhang Y
Matthews H
Montgomery W
Shih HY
Jiang J
Jones M
Baras A
Shuldiner A
Gonzaga-Jauregui C
Snapper SB
Muise AM
Shouval DS
Ozen A
Pan KT
Wu C
Lenardo MJ
Source :: Cell [Cell] 2022 Mar 31; Vol. 185 (7), pp. 1172-1188.e28. Date of Electronic Publication: 2022 Mar 17.
Publication Year :: 2022
Abstract: Intestinal mucus forms the first line of defense against bacterial invasion while providing nutrition to support microbial symbiosis. How the host controls mucus barrier integrity and commensalism is unclear. We show that terminal sialylation of glycans on intestinal mucus by ST6GALNAC1 (ST6), the dominant sialyltransferase specifically expressed in goblet cells and induced by microbial pathogen-associated molecular patterns, is essential for mucus integrity and protecting against excessive bacterial proteolytic degradation. Glycoproteomic profiling and biochemical analysis of ST6 mutations identified in patients show that decreased sialylation causes defective mucus proteins and congenital inflammatory bowel disease (IBD). Mice harboring a patient ST6 mutation have compromised mucus barriers, dysbiosis, and susceptibility to intestinal inflammation. Based on our understanding of the ST6 regulatory network, we show that treatment with sialylated mucin or a Foxo3 inhibitor can ameliorate IBD.<br />Competing Interests: Declaration of interests The authors declare no competing interests.<br /> (Copyright © 2022. Published by Elsevier Inc.)