| Literature DB >> 31068441 |
Tieshi Li1,2, Susan Chubinskaya1, Alessandra Esposito1,2, Xin Jin1,3, Lidia Tagliafierro4, Richard Loeser5, Arnavaz A Hakimiyan1, Lara Longobardi5, Huseyin Ozkan5,6, Anna Spagnoli7,2.
Abstract
Mechanisms that govern the shift from joint homeostasis to osteoarthritis (OA) remain unknown. Here, we identify a pathway used for joint development and homeostasis, and its role in OA. Using a combination of transgenic, pharmacological, and surgical conditions in mouse and human tissues, we found that TGF-β signaling promotes joint homeostasis through regulation of the IL-36 family. We identified IL-36 receptor antagonist (IL-36 in mice and IL-36RN in humans) as a potential disease-modifying OA drug. Specifically, OA development was associated with IL-36α up-regulation and IL-36Ra down-regulation in mice with tissue-specific postnatally induced ablation of Tgfbr2, mice treated with a TGF-β signaling inhibitor, mice with posttraumatic OA, and aging mice with naturally occurring OA. In human cartilage, OA severity was associated with decreased TGFBR2 and IL-36RN, whereas IL-36α increased. Functionally, intra-articular treatment with IL-36Ra attenuated OA development in mice, and IL-36RN reduced MMP13 in human OA chondrocytes. These findings highlight the relevance of TGFBR2-IL-36 interplay in joint homeostasis and IL-36RN as a potential therapeutic agent for OA.Entities:
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Year: 2019 PMID: 31068441 PMCID: PMC7102613 DOI: 10.1126/scitranslmed.aan2585
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956