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박찬영

Park, Chan Young
Calcium Dynamics Lab.
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ITGBL1 modulates integrin activity to promote cartilage formation and protect against arthritis.

Author(s)
Song, Eun KyungJeon, JiminJang, Dong GilKim, Ha EunSim, Hyo JungKwon, Keun YeongMedina-Ruiz, SofiaJang, Hyun-JunLee, Ah ReumRho, Jun GiLee, Hyun-ShikKim, Seok JungPark, Chan YoungMyung, KyungjaeKim, WookKwon, TaejoonYang, SiyoungPark, Tae Joo
Issued Date
2018-10
DOI
10.1126/scitranslmed.aam7486
URI
https://scholarworks.unist.ac.kr/handle/201301/24963
Fulltext
http://stm.sciencemag.org/content/10/462/eaam7486
Citation
SCIENCE TRANSLATIONAL MEDICINE, v.10, no.462, pp.eaam7486
Abstract
Developing and mature chondrocytes constantly interact with and remodel the surrounding extracellular matrix (ECM). Recent research indicates that integrin-ECM interaction is differentially regulated during cartilage formation (chondrogenesis). Integrin signaling is also a key source of the catabolic reactions responsible for joint destruction in both rheumatoid arthritis and osteoarthritis. However, we do not understand how chondrocytes dynamically regulate integrin signaling in such an ECM-rich environment. Here, we found that developing chondrocytes express integrin-β-like 1 (Itgbl1) at specific stages, inhibiting integrin signaling and promoting chondrogenesis. Unlike cytosolic integrin inhibitors, ITGBL1 is secreted and physically interacts with integrins to down-regulate activity. We observed that Itgbl1 expression was strongly reduced in the damaged articular cartilage of patients with osteoarthritis (OA). Ectopic expression of Itgbl1 protected joint cartilage against OA development in the destabilization of the medial meniscus-induced OA mouse model. Our results reveal ITGBL1 signaling as an underlying mechanism of protection against destructive cartilage disorders and suggest the potential therapeutic utility of targeting ITGBL1 to modulate integrin signaling in human disease.
Publisher
AMER ASSOC ADVANCEMENT SCIENCE
ISSN
1946-6234
Keyword
CRANIOFACIAL DEVELOPMENTMATRIX INTERACTIONSFOCAL ADHESION KINASEMESENCHYMAL STEM-CELLSCALCIUM-BINDING SITEEGF-LIKE DOMAINARTICULAR CHONDROCYTESFIBRONECTIN FRAGMENTSGENE-EXPRESSIONOSTEOARTHRITIC CARTILAGE

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