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Single-chain variable fragment albumin fusions bind the neonatal Fc receptor (FcRn) in a species dependent manner: implications for in vivo half-life evaluation of albumin-fusion therapeutics.

J Biol Chem.. 2013-07; 
Andersen JT, Cameron J, Plumridge A, Evans L, Sleep D, Sandlie I. Rikshospitalet University Hospital, Norway.
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摘要

Albumin has a serum half-life of three weeks in humans. This has been utilized to extend the serum persistence of biopharmaceuticals that are fused to albumin. In light of the fact that the neonatal Fc receptor (FcRn) is a key regulator of albumin homeostasis, it is crucial to address how fusion of therapeutics to albumin impacts binding to FcRn. Here, we report on a detailed molecular investigation on how genetic fusion of a short peptide or an scFv fragment to human serum albumin (HSA) influences pH-dependent binding to FcRn from mouse, rat, monkey and human. We have found that fusion to the N- or C-terminal end of HSA only slightly reduces receptor binding, where the most noticeable effect is seen after fusi... More

关键词

Albumin; Animal models; Antibody engineering; Bioengineering; Drug delivery; Pharmacokinetics; Receptor recycling; pH regulation