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Anti-Carcinoembryonic Antigen Single-Chain Variable Fragment Antibody Variants Bind Mouse And Human Neonatal Fc Receptor With Different Affinities That Reveal Distinct Cross-Species Differences In Serum Half-Life.

J Biol Chem.. 2012-06;  287(27):22927 - 22937
Jan Terje Andersen, Stian Foss, Vania E. Kenanova, Tove Olafsen, Ingvild S. Leikfoss, Derry C. Roopenian, Anna M. Wu, and Inger Sandlie. Centre for Immune Regulation and Department of Molecular Biosciences, University of Oslo, N-0316 Oslo, Norway.
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摘要

Serum half-life of IgG is controlled by the neonatal Fc receptor (FcRn) that interacts with the IgG Fc region and may be increased or decreased as a function of altered FcRn binding. Preclinical evaluations of modified IgGs are frequently carried out in mice, but such IgGs may bind differently to mouse and human FcRn (mFcRn and hFcRn). Here, we report a detailed characterization of a matched set of mouse-human chimeric T84.66 scFv-Fc variants with specificity for the tumor carcinoembryonic antigen and mutations in the FcRn-binding site. Binding to soluble mFcRn and hFcRn was measured using in vitro assays, and the results were compared with blood clearance in vivo in normal (mFcRn bearing) and hFcRn transgenic ... More

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