朱玲新

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Personal Information

Supervisor of Master's Candidates

Supervisor of Doctorate Candidates

  • E-Mail:

  • School/Department:

    口腔医学院
  • Administrative Position:

    教学办公室副主任
  • Education Level:

    With Certificate of Graduation for Doctorate Study
  • Business Address:

    武汉大学口腔医学院
  • Gender:

    Male
  • Contact Information:

    lingxin.zhu@whu.edu.cn
  • Status:

    Employed
  • Alma Mater:

    武汉大学
  • Teacher College:

    School of Stomatology (Hospital of Stomatology, Wuhan University)
  • Discipline:

    Clinical Stomatology

Other Contact Information

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  • PostalAddress:

  • Email:

Paper Publications

Current position: Home > Scientific Research > Paper Publications

Osteoclast-mediated bone resorption is controlled by a compensatory network of secreted and membrane-tethered metalloproteinases

  • Date:2024-10-26  Hits:Times
  • DOI number:  

    10.1126/scitranslmed.aaw6143
  • Journal:  

    Sci Transl Med
  • Abstract:  

    Osteoclasts actively remodel both the mineral and proteinaceous components of bone during normal growth and development as well as pathologic states ranging from osteoporosis to bone metastasis. The cysteine proteinase cathepsin K confers osteoclasts with potent type I collagenolytic activity; however, cathepsin K-null mice, as well as cathepsin K-mutant humans, continue to remodel bone and degrade collagen by as-yet-undefined effectors. Here, we identify a cathepsin K-independent collagenolytic system in osteoclasts that is composed of a functionally redundant network of the secreted matrix metalloproteinase MMP9 and the membrane-anchored matrix metalloproteinase MMP14. Unexpectedly, whereas deleting either of the proteinases individually leaves bone resorption intact, dual targeting of Mmp9 and Mmp14 inhibited the resorptive activity of mouse osteoclasts in vitro and in vivo and human osteoclasts in vitro. In vivo, Mmp9/Mmp14 conditional double-knockout mice exhibited marked increases in bone density and displayed a highly protected status against either parathyroid hormone- or ovariectomy-induced pathologic bone loss. Together, these studies characterize a collagenolytic system operative in mouse and human osteoclasts and identify the MMP9/MMP14 axis as a potential target for therapeutic interventions for bone-wasting disease states.
  • Co-author:  

    Tang Y, Li XY, Keller ET, Yang J, Cho JS, Feinberg TY
  • Correspondence Author:  

    Weiss SJ
  • Volume:  

    12
  • Issue:  

    529
  • Page Number:  

    eaaw6143
  • Translation or Not:  

    no
  • Date of Publication:  

    2020-02-25
  • Included Journals:  

    SCI