| Literature DB >> 27704775 |
Yan Liu1, Ying Wang1, Yong Zhang1, Tao Liu2, Haiqun Jia1, Huafei Zou1, Qiangwei Fu1, Yuhan Zhang1, Lucy Lu1, Elizabeth Chao1, Holly Parker1, Van Nguyen-Tran1, Weijun Shen1, Danling Wang1, Peter G Schultz1,2, Feng Wang1.
Abstract
Recent studies have suggested that modulation of two or more signaling pathways can achieve substantial weight loss and glycemic stability. We have developed an approach to the generation of bifunctional antibody agonists that activate leptin receptor and GLP-1 receptor. Leptin was fused into the complementarity determining region 3 loop of the light chain alone, or in combination with exendin-4 (EX4) fused at the N-terminus of the heavy chain of Herceptin. The antibody fusions exhibit similar or increased in vitro activities on their cognate receptors, but 50-100-fold longer circulating half-lives in rodents compared to the corresponding native peptides/proteins. The efficacy of the leptin/EX4 dual antibody fusion on weight loss, especially fat mass loss, was enhanced in ob/ob mice and DIO mice compared to the antibody fusion of either EX4 or leptin alone. This work demonstrates the versatility of this combinatorial fusion strategy for generating dual antibody agonists with long half-lives.Entities:
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Year: 2016 PMID: 27704775 PMCID: PMC5148668 DOI: 10.1021/acschembio.6b00630
Source DB: PubMed Journal: ACS Chem Biol ISSN: 1554-8929 Impact factor: 5.100