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Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice

The knowledge of osteoarthritis (OA) has nowadays been extended from a focalized cartilage disorder to a multifactorial disease. Although recent investigations have reported that infrapatellar fat pad (IPFP) can trigger inflammation in the knee joint, the mechanisms behind the role of IPFP on knee O...

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Autores principales: Dai, Bingyang, Zhu, Yuwei, Li, Xu, Liang, Zuru, Xu, Shunxiang, Zhang, Shian, Zhang, Zhe, Bai, Shanshan, Tong, Wenxue, Cao, Mingde, Li, Ye, Zhu, Xiaobo, Liu, Wei, Zhang, Yuantao, Chang, Liang, Yung, Patrick Shu‐hang, Ki‐wai Ho, Kevin, Xu, Jiankun, Ngai, To, Qin, Ling
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10401113/
https://www.ncbi.nlm.nih.gov/pubmed/37218542
http://dx.doi.org/10.1002/advs.202300897
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author Dai, Bingyang
Zhu, Yuwei
Li, Xu
Liang, Zuru
Xu, Shunxiang
Zhang, Shian
Zhang, Zhe
Bai, Shanshan
Tong, Wenxue
Cao, Mingde
Li, Ye
Zhu, Xiaobo
Liu, Wei
Zhang, Yuantao
Chang, Liang
Yung, Patrick Shu‐hang
Ki‐wai Ho, Kevin
Xu, Jiankun
Ngai, To
Qin, Ling
author_facet Dai, Bingyang
Zhu, Yuwei
Li, Xu
Liang, Zuru
Xu, Shunxiang
Zhang, Shian
Zhang, Zhe
Bai, Shanshan
Tong, Wenxue
Cao, Mingde
Li, Ye
Zhu, Xiaobo
Liu, Wei
Zhang, Yuantao
Chang, Liang
Yung, Patrick Shu‐hang
Ki‐wai Ho, Kevin
Xu, Jiankun
Ngai, To
Qin, Ling
author_sort Dai, Bingyang
collection PubMed
description The knowledge of osteoarthritis (OA) has nowadays been extended from a focalized cartilage disorder to a multifactorial disease. Although recent investigations have reported that infrapatellar fat pad (IPFP) can trigger inflammation in the knee joint, the mechanisms behind the role of IPFP on knee OA progression remain to be defined. Here, dysregulated osteopontin (OPN) and integrin β3 signaling are found in the OA specimens of both human and mice. It is further demonstrated that IPFP‐derived OPN participates in OA progression, including activated matrix metallopeptidase 9 in chondrocyte hypertrophy and integrin β3 in IPFP fibrosis. Motivated by these findings, an injectable nanogel is fabricated to provide sustained release of siRNA Cd61 ((RGD−)Nanogel/siRNA Cd61) that targets integrins. The (RGD−)Nanogel possesses excellent biocompatibility and desired targeting abilities both in vitro and in vivo. Local injection of (RGD−)Nanogel/siRNA Cd61 robustly alleviates the cartilage degeneration, suppresses the advancement of tidemark, and reduces the subchondral trabecular bone mass in OA mice. Taken together, this study provides an avenue for developing (RGD−)Nanogel/siRNA Cd61 therapy to mitigate OA progression via blocking OPN‐integrin β3 signaling in IPFP.
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spelling pubmed-104011132023-08-05 Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice Dai, Bingyang Zhu, Yuwei Li, Xu Liang, Zuru Xu, Shunxiang Zhang, Shian Zhang, Zhe Bai, Shanshan Tong, Wenxue Cao, Mingde Li, Ye Zhu, Xiaobo Liu, Wei Zhang, Yuantao Chang, Liang Yung, Patrick Shu‐hang Ki‐wai Ho, Kevin Xu, Jiankun Ngai, To Qin, Ling Adv Sci (Weinh) Research Articles The knowledge of osteoarthritis (OA) has nowadays been extended from a focalized cartilage disorder to a multifactorial disease. Although recent investigations have reported that infrapatellar fat pad (IPFP) can trigger inflammation in the knee joint, the mechanisms behind the role of IPFP on knee OA progression remain to be defined. Here, dysregulated osteopontin (OPN) and integrin β3 signaling are found in the OA specimens of both human and mice. It is further demonstrated that IPFP‐derived OPN participates in OA progression, including activated matrix metallopeptidase 9 in chondrocyte hypertrophy and integrin β3 in IPFP fibrosis. Motivated by these findings, an injectable nanogel is fabricated to provide sustained release of siRNA Cd61 ((RGD−)Nanogel/siRNA Cd61) that targets integrins. The (RGD−)Nanogel possesses excellent biocompatibility and desired targeting abilities both in vitro and in vivo. Local injection of (RGD−)Nanogel/siRNA Cd61 robustly alleviates the cartilage degeneration, suppresses the advancement of tidemark, and reduces the subchondral trabecular bone mass in OA mice. Taken together, this study provides an avenue for developing (RGD−)Nanogel/siRNA Cd61 therapy to mitigate OA progression via blocking OPN‐integrin β3 signaling in IPFP. John Wiley and Sons Inc. 2023-05-23 /pmc/articles/PMC10401113/ /pubmed/37218542 http://dx.doi.org/10.1002/advs.202300897 Text en © 2023 The Authors. Advanced Science published by Wiley‐VCH GmbH https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Dai, Bingyang
Zhu, Yuwei
Li, Xu
Liang, Zuru
Xu, Shunxiang
Zhang, Shian
Zhang, Zhe
Bai, Shanshan
Tong, Wenxue
Cao, Mingde
Li, Ye
Zhu, Xiaobo
Liu, Wei
Zhang, Yuantao
Chang, Liang
Yung, Patrick Shu‐hang
Ki‐wai Ho, Kevin
Xu, Jiankun
Ngai, To
Qin, Ling
Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice
title Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice
title_full Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice
title_fullStr Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice
title_full_unstemmed Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice
title_short Blockage of Osteopontin‐Integrin β3 Signaling in Infrapatellar Fat Pad Attenuates Osteoarthritis in Mice
title_sort blockage of osteopontin‐integrin β3 signaling in infrapatellar fat pad attenuates osteoarthritis in mice
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10401113/
https://www.ncbi.nlm.nih.gov/pubmed/37218542
http://dx.doi.org/10.1002/advs.202300897
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