TY - JOUR
T1 - Epitope-specific monoclonal antibodies to FSHβ increase bone mass
AU - Ji, Yaoting
AU - Liu, Peng
AU - Yuen, Tony
AU - Haider, Shozeb
AU - He, Jiahuan
AU - Romero, Raquel
AU - Chen, Hao
AU - Bloch, Madison
AU - Kim, Se Min
AU - Lizneva, Daria
AU - Munshi, Lubna
AU - Zhou, Chunxue
AU - Lu, Ping
AU - Iqbal, Jameel
AU - Cheng, Zhen
AU - New, Maria I.
AU - Hsueh, Aaron J.
AU - Bian, Zhuan
AU - Rosen, Clifford J.
AU - Sun, Li
AU - Zaidi, Mone
N1 - Publisher Copyright:
© 2018 National Academy of Sciences. All Rights Reserved.
PY - 2018/2/27
Y1 - 2018/2/27
N2 - Pituitary hormones have long been thought solely to regulate single targets. Challenging this paradigm, we discovered that both anterior and posterior pituitary hormones, including FSH, had other functions in physiology. We have shown that FSH regulates skeletal integrity, and, more recently, find that FSH inhibition reduces body fat and induces thermogenic adipose tissue. A polyclonal antibody raised against a short, receptor-binding epitope of FSHβ was found not only to rescue bone loss postovariectomy, but also to display marked antiobesity and probeiging actions. Questioning whether a single agent could be used to treat two medical conditions of public health importance-osteoporosis and obesity-we developed two further monoclonal antibodies, Hf2 and Mf4, against computationally defined receptor-binding epitopes of FSHβ. Hf2 has already been shown to reduce body weight and fat mass and cause beiging in mice on a high-fat diet. Here, we show that Hf2, which binds mouse Fsh in immunoprecipitation assays, also increases cortical thickness and trabecular bone volume, and microstructural parameters, in sham-operated and ovariectomized mice, noted on microcomputed tomography. This effect was largely recapitulated with Mf4, which inhibited bone resorption by osteoclasts and stimulated new bone formation by osteoblasts. These effects were exerted in the absence of alterations in serum estrogen in wild-type mice. We also reconfirm the existence of Fshrs in bone by documenting the specific binding of fluorescently labeled FSH, FSH-CH, in vivo. Our study provides the framework for the future development of an FSH-based therapeutic that could potentially target both bone and fat.
AB - Pituitary hormones have long been thought solely to regulate single targets. Challenging this paradigm, we discovered that both anterior and posterior pituitary hormones, including FSH, had other functions in physiology. We have shown that FSH regulates skeletal integrity, and, more recently, find that FSH inhibition reduces body fat and induces thermogenic adipose tissue. A polyclonal antibody raised against a short, receptor-binding epitope of FSHβ was found not only to rescue bone loss postovariectomy, but also to display marked antiobesity and probeiging actions. Questioning whether a single agent could be used to treat two medical conditions of public health importance-osteoporosis and obesity-we developed two further monoclonal antibodies, Hf2 and Mf4, against computationally defined receptor-binding epitopes of FSHβ. Hf2 has already been shown to reduce body weight and fat mass and cause beiging in mice on a high-fat diet. Here, we show that Hf2, which binds mouse Fsh in immunoprecipitation assays, also increases cortical thickness and trabecular bone volume, and microstructural parameters, in sham-operated and ovariectomized mice, noted on microcomputed tomography. This effect was largely recapitulated with Mf4, which inhibited bone resorption by osteoclasts and stimulated new bone formation by osteoblasts. These effects were exerted in the absence of alterations in serum estrogen in wild-type mice. We also reconfirm the existence of Fshrs in bone by documenting the specific binding of fluorescently labeled FSH, FSH-CH, in vivo. Our study provides the framework for the future development of an FSH-based therapeutic that could potentially target both bone and fat.
KW - Antiobesity
KW - FSH monoclonal antibody
KW - FSH polyclonal antibody
KW - FSH receptor
KW - Osteoporosis treatment
UR - http://www.scopus.com/inward/record.url?scp=85042641127&partnerID=8YFLogxK
U2 - 10.1073/pnas.1718144115
DO - 10.1073/pnas.1718144115
M3 - Article
C2 - 29440419
AN - SCOPUS:85042641127
SN - 0027-8424
VL - 115
SP - 2192
EP - 2197
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 9
ER -