| Literature DB >> 30644553 |
Dongye Zhang1, Mariana Miranda1, Xiaofei Li1, Jiangmeng Han1, Yueli Sun1, Nancy Rojas1, Shan He2, Minyi Hu1, Liangjun Lin1, Xiaodong Li3, Hua Zhu Ke4, Yi-Xian Qin1.
Abstract
Prolonged mechanical unloading in bedridden patients and concurrent hormonal dysregulation represents the cause of one of the severest forms of osteoporosis, a condition for which there are very few efficacious interventions available to date. Sclerostin, a Wnt antagonist, acts as a negative regulator of bone formation. Sclerostin antibody (Scl-Ab)-mediated blockade of sclerostin can dramatically enhance bone formation and reduce bone resorption. This study was designed to investigate the therapeutic effect of the Scl-Ab on severe bone loss induced by concurrent mechanical unloading and estrogen deficiency in a hindlimb-suspended and ovariectomized rat model, and to study the cellular mechanisms underlying severe osteoporosis and Scl-Ab action. Unloading and ovariectomy resulted in severe loss of trabecular and cortical bone mass and strength; Scl-Ab can significantly counteract the deterioration of bone in unloaded and/or ovariectomized rats, with noticeably increased cortical bone formation. Scanning electron microscopy analysis revealed that unloading and ovariectomy lead to multiple morphological and structural abnormalities of osteocytes in cortical bone and the abnormalities were abolished by Scl-Ab administration. This study extends our previous conclusion that Scl-Ab represents a promising therapeutic approach for severe bone loss that occurs after being exposed to estrogen deficiency and prolonged mechanical unloading.Entities:
Keywords: estrogen deficiency; mechanical unloading; osteocyte; scanning electron microscopy; sclerostin antibody; severe osteoporosis
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Year: 2019 PMID: 30644553 PMCID: PMC6465143 DOI: 10.1111/nyas.13991
Source DB: PubMed Journal: Ann N Y Acad Sci ISSN: 0077-8923 Impact factor: 5.691