PTPN2 links colonic and joint inflammation in experimental autoimmune arthritis
Wan-Chen Hsieh, … , Stephanie M. Stanford, Nunzio Bottini
Wan-Chen Hsieh, … , Stephanie M. Stanford, Nunzio Bottini
Published October 15, 2020
Citation Information: JCI Insight. 2020;5(20):e141868. https://doi.org/10.1172/jci.insight.141868.
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Research Article Inflammation

PTPN2 links colonic and joint inflammation in experimental autoimmune arthritis

Abstract

Loss-of-function variants of protein tyrosine phosphatase non-receptor type 2 (PTPN2) enhance risk of inflammatory bowel disease and rheumatoid arthritis; however, whether the association between PTPN2 and autoimmune arthritis depends on gut inflammation is unknown. Here we demonstrate that induction of subclinical intestinal inflammation exacerbates development of autoimmune arthritis in SKG mice. Ptpn2-haploinsufficient SKG mice — modeling human carriers of disease-associated variants of PTPN2 — displayed enhanced colitis-induced arthritis and joint accumulation of Tregs expressing RAR-related orphan receptor γT (RORγt) — a gut-enriched Treg subset that can undergo conversion into FoxP3–IL-17+ arthritogenic exTregs. SKG colonic Tregs underwent higher conversion into arthritogenic exTregs when compared with peripheral Tregs, which was exacerbated by haploinsufficiency of Ptpn2. Ptpn2 haploinsufficiency led to selective joint accumulation of RORγt-expressing Tregs expressing the colonic marker G protein–coupled receptor 15 (GPR15) in arthritic mice and selectively enhanced conversion of GPR15+ Tregs into exTregs in vitro and in vivo. Inducible Treg-specific haploinsufficiency of Ptpn2 enhanced colitis-induced SKG arthritis and led to specific joint accumulation of GPR15+ exTregs. Our data validate the SKG model for studies at the interface between intestinal and joint inflammation and suggest that arthritogenic variants of PTPN2 amplify the link between gut inflammation and arthritis through conversion of colonic Tregs into exTregs.

Authors

Wan-Chen Hsieh, Mattias N.D. Svensson, Martina Zoccheddu, Michael L. Tremblay, Shimon Sakaguchi, Stephanie M. Stanford, Nunzio Bottini

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Figure 5

Ptpn2 haploinsufficiency causes enhanced conversion of GPR15+ Tregs in vitro and in vivo.

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Ptpn2 haploinsufficiency causes enhanced conversion of GPR15+ Tregs in ...
(A) Frequency of GPR15-expressing Tregs (CD4+FoxP3+GPR15+) among CD4+ T cells in spleen (Sp), lymph nodes (LN) and colons of prearthritic SKG mice (n = 7). (B and C) Number of GPR15+ and GPR15 RORγt+ Tregs (CD4+RORγt+FoxP3+ GPR15+ or GPR15) and RORγt+FoxP3CD4+ T cells (CD4+RORγt+FoxP3 GPR15+ or GPR15) in ankles of Ptpn2+/+ (n = 8) and Ptpn2+/– (n = 12) SKG mice with mannan-induced arthritis at day 49 shown in Supplemental Figure 4. (D) Frequency of IL-17A–producing exTregs (CD4+IL-17A+FoxP3) after in vitro conversion of GPR15+ and GPR15 Tregs isolated from Ptpn2+/+ (n = 5) and Ptpn2+/– (n = 5) FoxP3EGFP+ SKG mice. (EG) Cotransfer of CD45.1 SKG CD4+CD25 Ptpn2+/+ Teffs together with GPR15+ Ptpn2+/+ (n = 10) or Ptpn2+/– (n = 9) Tregs (CD4+FoxP3EGFP+GPR15+) or GPR15 Ptpn2+/+ (n = 10) or Ptpn2+/– (n = 10) Tregs (CD4+FoxP3EGFP+GPR15) into Rag2-KO mice. Arthritis was induced 1 week after cell transfer by an intraperitoneal injection of mannan. (E) Schematic for adoptive transfer experiment. (F) Clinical score and change in ankle swelling in Rag2-KO recipient mice. (G) Frequency of IL-17–producing exTregs (CD45.2+CD4+IL-17A+Foxp3) in lymph nodes and ankles of arthritic recipient mice on day 28. (H) Frequency of Th17 (CD45.1+CD4+IL-17A+FoxP3) among CD45.1 Teffs in lymph nodes and ankles of arthritic recipient mice on day 28. Compiled data from at least 2 (A) or 3 (DH) independent experiments are shown. Each symbol in AD, G, and H represents an individual mouse. Graphs show mean ± SEM.*P < 0.05, **P < 0.01, ***P < 0.001 by 1-way ANOVA (A), unpaired t test (B and C), Mann-Whitney U test (F), or 2-way ANOVA (D, G, and H).