SMURF2 regulates bone homeostasis by disrupting SMAD3 interaction with vitamin D receptor in osteoblasts

Zhan Xu,Matthew B. Greenblatt,Guang Yan,Heng Feng,Jun Sun,Sutada Lotinun,Nicholas Brady,Roland Baron,Laurie H. Glimcher,Weiguo Zou

SMURF2 regulates bone homeostasis by disrupting SMAD3 interaction with vitamin D receptor in osteoblasts

2017

Zhan Xu
Matthew B. Greenblatt
Guang Yan
Heng Feng
Jun Sun
Sutada Lotinun
Nicholas Brady
Roland Baron
Laurie H. Glimcher
Weiguo Zou

The balance between osteoclast and osteoblast-mediated bone turnover is essential for bone health and homeostasis. Here the authors show that both germline and osteoblast-specific Smurf2-deficient mice have osteoporosis as a result of increased osteoblast RANKL production and excess osteoclastogenesis.

Keywords:

Bone health
Bone remodeling
Osteoporosis
Homeostasis
Germline
Osteoclast
Osteoblast
Biology
Calcitriol receptor
Endocrinology
Internal medicine
RANKL
Phenotype

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