An engineered human Fc domain that behaves like a pH-toggle switch for ultra-long circulation persistence

Author:

Lee Chang-HanORCID,Kang Tae HyunORCID,Godon Ophélie,Watanabe MakikoORCID,Delidakis GeorgeORCID,Gillis Caitlin M.ORCID,Sterlin Delphine,Hardy David,Cogné Michel,Macdonald Lynn E.,Murphy Andrew J.ORCID,Tu Naxin,Lee JiwonORCID,McDaniel Jonathan R.,Makowski Emily,Tessier Peter M.,Meyer Aaron S.ORCID,Bruhns Pierre,Georgiou George

Abstract

Abstract The pharmacokinetic properties of antibodies are largely dictated by the pH-dependent binding of the IgG fragment crystallizable (Fc) domain to the human neonatal Fc receptor (hFcRn). Engineered Fc domains that confer a longer circulation half-life by virtue of more favorable pH-dependent binding to hFcRn are of great therapeutic interest. Here we developed a pH Toggle switch Fc variant containing the L309D/Q311H/N434S (DHS) substitutions, which exhibits markedly improved pharmacokinetics relative to both native IgG1 and widely used half-life extension variants, both in conventional hFcRn transgenic mice and in new knock-in mouse strains. engineered specifically to recapitulate all the key processes relevant to human antibody persistence in circulation, namely: (i) physiological expression of hFcRn, (ii) the impact of hFcγRs on antibody clearance and (iii) the role of competing endogenous IgG. DHS-IgG retains intact effector functions, which are important for the clearance of target pathogenic cells and also has favorable developability.

Funder

The Clayton Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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