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  • A human endothelial cell-based recycling assay for screening of FcRn targeted molecules.

A human endothelial cell-based recycling assay for screening of FcRn targeted molecules.

Nature communications (2018-02-13)
Algirdas Grevys, Jeannette Nilsen, Kine M K Sand, Muluneh B Daba, Inger Øynebråten, Malin Bern, Martin B McAdam, Stian Foss, Tilman Schlothauer, Terje E Michaelsen, Gregory J Christianson, Derry C Roopenian, Richard S Blumberg, Inger Sandlie, Jan Terje Andersen
摘要

Albumin and IgG have remarkably long serum half-lives due to pH-dependent FcRn-mediated cellular recycling that rescues both ligands from intracellular degradation. Furthermore, increase in half-lives of IgG and albumin-based therapeutics has the potential to improve their efficacies, but there is a great need for robust methods for screening of relative FcRn-dependent recycling ability. Here, we report on a novel human endothelial cell-based recycling assay (HERA) that can be used for such pre-clinical screening. In HERA, rescue from degradation depends on FcRn, and engineered ligands are recycled in a manner that correlates with their half-lives in human FcRn transgenic mice. Thus, HERA is a novel cellular assay that can be used to predict how FcRn-binding proteins are rescued from intracellular degradation.

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Sigma-Aldrich
抗 人 IgG(Fc 特异性)-碱性磷酸酶 山羊抗, affinity isolated antibody, buffered aqueous solution
Sigma-Aldrich
抗-白蛋白 山羊抗, fractionated antiserum, lyophilized
Sigma-Aldrich
抗 小鼠 IgG(Fc 特异性)-碱性磷酸酶 山羊抗, affinity isolated antibody, buffered aqueous solution