Distinct inflammatory Th17 subsets emerge in autoimmunity and infection

Ronald J Bouch; Jing Zhang; Brandi C Miller; Caroline J Robbins; Timothy H Mosher; Wencheng Li; Sergey A Krupenko; Ravinder Nagpal; Jun Zhao; Richard S Bloomfeld; Yong Lu; Mikhail A Nikiforov; Qianqian Song; Zhiheng He

doi:10.1084/jem.20221911

Distinct inflammatory Th17 subsets emerge in autoimmunity and infection

Ronald J Bouch, Jing Zhang, Brandi C Miller, Caroline J Robbins, Timothy H Mosher, Wencheng Li, Sergey A Krupenko, Ravinder Nagpal, Jun Zhao, Richard S Bloomfeld, Yong Lu, Mikhail A Nikiforov, Qianqian Song, Zhiheng He

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Th17 cells play a critical role in both tissue homeostasis and inflammation during clearance of infections as well as autoimmune and inflammatory disorders. Despite numerous efforts to distinguish the homeostatic and inflammatory roles of Th17 cells, the mechanism underlying the divergent functions of inflammatory Th17 cells remains poorly understood. In this study, we demonstrate that the inflammatory Th17 cells involved in autoimmune colitis and those activated during colitogenic infection are distinguishable populations characterized by their differential responses to the pharmacological molecule, clofazimine (CLF). Unlike existing Th17 inhibitors, CLF selectively inhibits proautoimmune Th17 cells while preserving the functional state of infection-elicited Th17 cells partially by reducing the enzyme ALDH1L2. Overall, our study identifies two distinct subsets within the inflammatory Th17 compartment with distinct regulatory mechanisms. Furthermore, we highlight the feasibility to develop disease-promoting Th17 selective inhibitor for treating autoimmune diseases.

Original language	English (US)
Article number	e20221911
Journal	The Journal of experimental medicine
Volume	220
Issue number	10
DOIs	https://doi.org/10.1084/jem.20221911
State	Published - Oct 2 2023

Keywords

Humans
Autoimmunity
Th17 Cells
Autoimmune Diseases
Inflammation
Colitis

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.1084/jem.20221911

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title = "Distinct inflammatory Th17 subsets emerge in autoimmunity and infection",

abstract = "Th17 cells play a critical role in both tissue homeostasis and inflammation during clearance of infections as well as autoimmune and inflammatory disorders. Despite numerous efforts to distinguish the homeostatic and inflammatory roles of Th17 cells, the mechanism underlying the divergent functions of inflammatory Th17 cells remains poorly understood. In this study, we demonstrate that the inflammatory Th17 cells involved in autoimmune colitis and those activated during colitogenic infection are distinguishable populations characterized by their differential responses to the pharmacological molecule, clofazimine (CLF). Unlike existing Th17 inhibitors, CLF selectively inhibits proautoimmune Th17 cells while preserving the functional state of infection-elicited Th17 cells partially by reducing the enzyme ALDH1L2. Overall, our study identifies two distinct subsets within the inflammatory Th17 compartment with distinct regulatory mechanisms. Furthermore, we highlight the feasibility to develop disease-promoting Th17 selective inhibitor for treating autoimmune diseases.",

keywords = "Humans, Autoimmunity, Th17 Cells, Autoimmune Diseases, Inflammation, Colitis",

author = "Bouch, {Ronald J} and Jing Zhang and Miller, {Brandi C} and Robbins, {Caroline J} and Mosher, {Timothy H} and Wencheng Li and Krupenko, {Sergey A} and Ravinder Nagpal and Jun Zhao and Bloomfeld, {Richard S} and Yong Lu and Nikiforov, {Mikhail A} and Qianqian Song and Zhiheng He",

note = "Funding Information: S.A. Krupenko is supported by the National Institutes of Health (NIH) grant R01DK117854. J. Zhang is supported by NIH grant R00DE028973. Q. Song is supported in part by the Bio-informatics Shared Resources under the National Cancer Institute Cancer Center Support Grant to the Comprehensive Cancer Center of Wake Forest University Health Sciences (P30CA012197). Z. He is supported by the NIH grant UL1TR001420, R21AI166159 and R01AI173277, and Errett Fisher Foundation award. R.J. Bouch was supported by NIH grant 5T32A1007401-28. Publisher Copyright: {\textcopyright} 2023 Bouch et al.",

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doi = "10.1084/jem.20221911",

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T1 - Distinct inflammatory Th17 subsets emerge in autoimmunity and infection

AU - Bouch, Ronald J

AU - Zhang, Jing

AU - Miller, Brandi C

AU - Robbins, Caroline J

AU - Mosher, Timothy H

AU - Li, Wencheng

AU - Krupenko, Sergey A

AU - Nagpal, Ravinder

AU - Zhao, Jun

AU - Bloomfeld, Richard S

AU - Lu, Yong

AU - Nikiforov, Mikhail A

AU - Song, Qianqian

AU - He, Zhiheng

N1 - Funding Information: S.A. Krupenko is supported by the National Institutes of Health (NIH) grant R01DK117854. J. Zhang is supported by NIH grant R00DE028973. Q. Song is supported in part by the Bio-informatics Shared Resources under the National Cancer Institute Cancer Center Support Grant to the Comprehensive Cancer Center of Wake Forest University Health Sciences (P30CA012197). Z. He is supported by the NIH grant UL1TR001420, R21AI166159 and R01AI173277, and Errett Fisher Foundation award. R.J. Bouch was supported by NIH grant 5T32A1007401-28. Publisher Copyright: © 2023 Bouch et al.

PY - 2023/10/2

Y1 - 2023/10/2

N2 - Th17 cells play a critical role in both tissue homeostasis and inflammation during clearance of infections as well as autoimmune and inflammatory disorders. Despite numerous efforts to distinguish the homeostatic and inflammatory roles of Th17 cells, the mechanism underlying the divergent functions of inflammatory Th17 cells remains poorly understood. In this study, we demonstrate that the inflammatory Th17 cells involved in autoimmune colitis and those activated during colitogenic infection are distinguishable populations characterized by their differential responses to the pharmacological molecule, clofazimine (CLF). Unlike existing Th17 inhibitors, CLF selectively inhibits proautoimmune Th17 cells while preserving the functional state of infection-elicited Th17 cells partially by reducing the enzyme ALDH1L2. Overall, our study identifies two distinct subsets within the inflammatory Th17 compartment with distinct regulatory mechanisms. Furthermore, we highlight the feasibility to develop disease-promoting Th17 selective inhibitor for treating autoimmune diseases.

AB - Th17 cells play a critical role in both tissue homeostasis and inflammation during clearance of infections as well as autoimmune and inflammatory disorders. Despite numerous efforts to distinguish the homeostatic and inflammatory roles of Th17 cells, the mechanism underlying the divergent functions of inflammatory Th17 cells remains poorly understood. In this study, we demonstrate that the inflammatory Th17 cells involved in autoimmune colitis and those activated during colitogenic infection are distinguishable populations characterized by their differential responses to the pharmacological molecule, clofazimine (CLF). Unlike existing Th17 inhibitors, CLF selectively inhibits proautoimmune Th17 cells while preserving the functional state of infection-elicited Th17 cells partially by reducing the enzyme ALDH1L2. Overall, our study identifies two distinct subsets within the inflammatory Th17 compartment with distinct regulatory mechanisms. Furthermore, we highlight the feasibility to develop disease-promoting Th17 selective inhibitor for treating autoimmune diseases.

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Distinct inflammatory Th17 subsets emerge in autoimmunity and infection

Abstract

Keywords

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