2020
DOI: 10.1038/s41413-020-00110-4
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Toward diagnostic relevance of the αVβ5, αVβ3, and αVβ6 integrins in OA: expression within human cartilage and spinal osteophytes

Abstract: We previously reported 18FPRGD2 uptake by the coxofemoral lining, intervertebral discs and facet joint osteophytes in OA using PET/SCAN imaging. However, the molecular mechanism by which the PRGD2 tracer interacts with joint tissues and osteophytes in OA remains unclear. As PRGD2 ligands are expected to belong to the RGD-specific integrin family, the purpose of this study was (i) to determine which integrin complexes display the highest affinity for PRGD2-based ligands, (ii) to analyze integrin expression in r… Show more

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Cited by 8 publications
(3 citation statements)
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“…A group of mechanosensing and mechanotransducing molecules may be regulated over PT-OA development and tune cellular mechano-sensitivity under abnormal joint mechanics and inflammation post-ACL-I. For instance, dysregulated integrin α V β 3 and their associated ligands may play essential roles in disrupting chondrocyte-ECM interactions over OA progression [ [47] , [48] , [49] ], as well as Piezo1 may be augmented via IL-1-mediated inflammatory patho-mechanisms [ 50 ]. This study has explored female mice but not male mice, also mechanically-induced chondrocyte death are quantified using living cells in the native tissues, ex vivo and in situ, post-ACL-injuries, but not compared with histological assays, such as TUNEL/Necrosis assays.…”
Section: Discussionmentioning
confidence: 99%
“…A group of mechanosensing and mechanotransducing molecules may be regulated over PT-OA development and tune cellular mechano-sensitivity under abnormal joint mechanics and inflammation post-ACL-I. For instance, dysregulated integrin α V β 3 and their associated ligands may play essential roles in disrupting chondrocyte-ECM interactions over OA progression [ [47] , [48] , [49] ], as well as Piezo1 may be augmented via IL-1-mediated inflammatory patho-mechanisms [ 50 ]. This study has explored female mice but not male mice, also mechanically-induced chondrocyte death are quantified using living cells in the native tissues, ex vivo and in situ, post-ACL-injuries, but not compared with histological assays, such as TUNEL/Necrosis assays.…”
Section: Discussionmentioning
confidence: 99%
“…A group of mechanosensing and mechanotransducing molecules may be regulated over PT-OA development and tune cellular mechano-sensitivity under abnormal joint mechanics and inflammation post-ACL-I. For instance, dysregulated integrin αVβ3 and their associated ligands may play essential roles in disrupting chondrocyte-ECM interactions over OA progression [77][78][79] , as well as Piezo1 may be augmented via IL-1-mediated inflammatory patho-mechanisms 80,81 . Future research will investigate the chondrocyte mechano-vulnerability based on mechanosensors and mechanotransducers and their local ECM properties over PT-OA development.…”
Section: Mechanical Property Of Ecm: Soften In Uni-acl-i Stiffen In Bi-acl-i At 8-weeks Post-injurymentioning
confidence: 99%
“…Integrins differ in tissue distribution and ligand identification. Recently, it has been reported that α V β 5 , α V β 3 , and α V β 6 interact with PRGD 2 , and their expression levels are increased in osteoarthritic cartilage and osteophytes 11 . Integrin α V β 6 interacts with molecules that contain the Arg-Gly-Asp (RGD) motif.…”
Section: Introductionmentioning
confidence: 99%