Literature DB >> 30602565

A new class of recombinant human albumin with multiple surface thiols exhibits stable conjugation and enhanced FcRn binding and blood circulation.

Karen Kræmmer Schelde1, Karl Nicholls2, Frederik Dagnæs-Hansen3, Karen Bunting2, Helen Rawsthorne2, Birgitte Andersen4, Christopher J A Finnis2, Miranda Williamson2, Jason Cameron2, Kenneth A Howard5.   

Abstract

Human serum albumin is an endogenous ligand transport protein whose long circulatory half-life is facilitated by engagement with the human cellular recycling neonatal Fc receptor (hFcRn). The single free thiol located at Cys-34 in domain I of albumin has been exploited for monoconjugation of drugs. In this work, we increased the drug-to-albumin ratio potential by engineering recombinant human albumin (rHSA) variants with varying hFcRn affinity to contain three free, conjugation-competent cysteines. Structural analysis was used to identify positions for cysteine introduction to maximize rHSA stability and formation of the conjugated product without affecting hFcRn binding. The thiol rHSA variants exhibited up to 95% monomeric stability over 24 months and retained hFcRn engagement compared with a WT unconjugated control demonstrated by Biolayer Interferometry. The additional cysteines were further introduced into a panel of rHSA variants engineered with different affinities for hFcRn. After conjugation with three Alexa Fluor 680 (AF680) fluorophores, hFcRn binding was similar to that of the original triple-thiol nonconjugated rHSA variants (0.88 and 0.25 μm for WT albumin with or without 3xAF680 respectively, and 0.04 and 0.02 μm for a high hFcRn-binding variant with or without 3xAF680, respectively). We also observed a 1.3-fold increase in the blood circulatory half-life of a high hFcRn-binding triple-thiol variant conjugated with AF680 (t ½ = 22.4 h) compared with its WT counterpart (t ½ = 17.3 h) in mice. Potential high drug-to-albumin ratios combined with high hFcRn engagement are attractive features of this new class of albumins that offer a paradigm shift for albumin-based drug delivery.
© 2019 Schelde et al.

Entities:  

Keywords:  Fc receptor; albumin; cysteine-mediated cross-linking; drug delivery; multidrug transporter; multifunctional protein; neonatal Fc receptor; pharmacokinetics; protein engineering; site-directed mutagenesis

Mesh:

Substances:

Year:  2019        PMID: 30602565      PMCID: PMC6416450          DOI: 10.1074/jbc.RA118.005870

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  26 in total

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Journal:  J Biol Chem       Date:  2009-12-14       Impact factor: 5.157

6.  Neonatal Fc Receptor Binding Tolerance toward the Covalent Conjugation of Payloads to Cysteine 34 of Human Albumin Variants.

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7.  Cellular recycling-driven in vivo half-life extension using recombinant albumin fusions tuned for neonatal Fc receptor (FcRn) engagement.

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Review 2.  Albumin uptake and processing by the proximal tubule: physiological, pathological, and therapeutic implications.

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