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Injectable Magnesium-Bisphosphonate MOF-Based Bone Adhesive Prevents Excessive Fibrosis for Osteoporotic Fracture Repair

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NIAID Data Ecosystem2026-05-02 收录
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https://www.ncbi.nlm.nih.gov/sra/SRP548419
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资源简介:
Current clinical approaches to promote osteoporotic fracture healing primarily target osteoclast biology, overlooking the negative regulatory role of fibroblasts in fracture healing. Perioperative bisphosphonates (BPs) used in anti-osteoporosis treatment for osteoporotic fractures have become a consensus worldwide. However, excessive fibrosis is induced simultaneously, leading to fracture non-union and atypical femur fractures. It is highly desirable to inhibit osteoclasts but block fibrosis. In this study, an magnesium ions (Mg2+)-BPs MOF-based bone adhesive material was designed to down-regulate SOST and weaken SOST/TGF-ß signaling pathway through Mg2+ through transcriptome analysis, thus inhibiting fibrotic differentiation and subsequent disordered mineralization. Overall design: In this study, a Mg-ALN MOF-based bone adhesive material was designed to antagonize the pathological characteristics of bone fibrosis induced by bisphosphonate (ALN) through Mg2+. Gel, ALN+Gel and Mg-ALN@Gel samples were analyzed by transcriptome sequencing. Mg2+ inhibited fibrotic differentiation by down-regulating SOST and attenuating SOST/TGF-ß signaling pathway.
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2025-08-12
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