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Targeting angiogenesis for fracture nonunion treatment in inflammatory disease

         

摘要

Atrophic fracture nonunion poses a significant clinical problem with limited therapeutic interventions.In this study,we developed a unique nonunion model with high clinical relevance using serum transfer-induced rheumatoid arthritis(RA).Arthritic mice displayed fracture nonunion with the absence of fracture callus,diminished angiogenesis and fibrotic scar tissue formation leading to the failure of biomechanical properties,representing the major manifestations of atrophic nonunion in the clinic.Mechanistically,we demonstrated that the angiogenesis defect observed in RA mice was due to the downregulation of SPP1 and CXCL12 in chondrocytes,as evidenced by the restoration of angiogenesis upon SPP1 and CXCL12 treatment in vitro.In this regard,we developed a biodegradable scaffold loaded with SPP1 and CXCL12,which displayed a beneficial effect on angiogenesis and fracture repair in mice despite the presence of inflammation.Hence,these findings strongly suggest that the sustained release of SPP1 and CXCL12 represents an effective therapeutic approach to treat impaired angiogenesis and fracture nonunion under inflammatory conditions.

著录项

  • 来源
    《骨研究:英文》 |2021年第3期|P.336-348|共13页
  • 作者单位

    Department of Orthopaedic Surgery School of Medicine Washington University St.Louis MO USA;

    Department of Orthopaedic Surgery School of Medicine Washington University St.Louis MO USADepartment of Orthopaedic Surgery the First Affiliated Hospital of Zhejiang Chinese Medical University Hangzhou ChinaInstitute of Orthopaedics and Traumatology the First Affiliated Hospital of Zhejiang Chinese Medical University Hangzhou China;

    Department of Mechanical Engineering&Materials Science School of Engineering Washington University St.Louis MO USA;

    Department of Mechanical Engineering&Materials Science School of Engineering Washington University St.Louis MO USA;

    Department of Orthopaedic Surgery School of Medicine Washington University St.Louis MO USA;

    Department of Orthopaedic Surgery School of Medicine Washington University St.Louis MO USA;

    Department of Orthopaedic Surgery School of Medicine Washington University St.Louis MO USAShriners Hospital for Children St.Louis MO USA;

    Department of Mechanical Engineering&Materials Science School of Engineering Washington University St.Louis MO USA;

    Department of Orthopaedic Surgery School of Medicine Washington University St.Louis MO USA;

  • 原文格式 PDF
  • 正文语种 chi
  • 中图分类 肿瘤学;
  • 关键词

    CXCL12; angiogenesis; impaired;

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