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First-in-class humanized FSH blocking antibody targets bone and fat.


ABSTRACT: Blocking the action of FSH genetically or pharmacologically in mice reduces body fat, lowers serum cholesterol, and increases bone mass, making an anti-FSH agent a potential therapeutic for three global epidemics: obesity, osteoporosis, and hypercholesterolemia. Here, we report the generation, structure, and function of a first-in-class, fully humanized, epitope-specific FSH blocking antibody with a K D of 7 nM. Protein thermal shift, molecular dynamics, and fine mapping of the FSH-FSH receptor interface confirm stable binding of the Fab domain to two of five receptor-interacting residues of the FSHβ subunit, which is sufficient to block its interaction with the FSH receptor. In doing so, the humanized antibody profoundly inhibited FSH action in cell-based assays, a prelude to further preclinical and clinical testing.

SUBMITTER: Gera S 

PROVIDER: S-EPMC7682550 | biostudies-literature | 2020 Nov

REPOSITORIES: biostudies-literature

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First-in-class humanized FSH blocking antibody targets bone and fat.

Gera Sakshi S   Sant Damini D   Haider Shozeb S   Korkmaz Funda F   Kuo Tan-Chun TC   Mathew Mehr M   Perez-Pena Helena H   Xie Honglin H   Chen Hao H   Batista Rogerio R   Ma Kejun K   Cheng Zhen Z   Hadelia Elina E   Robinson Cemre C   Macdonald Anne A   Miyashita Sari S   Williams Anthony A   Jebian Gregory G   Miyashita Hirotaka H   Gumerova Anisa A   Ievleva Kseniia K   Smith Pinar P   He Jiahuan J   Ryu Vitaly V   DeMambro Victoria V   Quinn Matthew A MA   Meseck Marcia M   Kim Se-Min SM   Kumar T Rajendra TR   Iqbal Jameel J   New Maria I MI   Lizneva Daria D   Rosen Clifford J CJ   Hsueh Aaron J AJ   Yuen Tony T   Zaidi Mone M  

Proceedings of the National Academy of Sciences of the United States of America 20201030 46


Blocking the action of FSH genetically or pharmacologically in mice reduces body fat, lowers serum cholesterol, and increases bone mass, making an anti-FSH agent a potential therapeutic for three global epidemics: obesity, osteoporosis, and hypercholesterolemia. Here, we report the generation, structure, and function of a first-in-class, fully humanized, epitope-specific FSH blocking antibody with a <i>K</i><sub>D</sub> of 7 nM. Protein thermal shift, molecular dynamics, and fine mapping of the  ...[more]

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