Optimised approach to albumin-drug conjugates using monobromomaleimide-C-2 linkers.
Archie WallKarl NichollsMikael B CaspersenStig SkrivergaardKenneth A HowardKersti KaruVijay ChudasamaJames Richard BakerPublished in: Organic & biomolecular chemistry (2020)
Conjugation of therapeutics to human serum albumin (HSA) using bromomaleimides represents a promising platform for half-life extension. We show here that the Cys-34 crevice substantially reduces the rate of serum stabilising maleimide hydrolysis in these conjugates, necessitating reagent optimisation. This improved reagent design is applied to the construction of an HSA-paclitaxel conjugate, preventing drug loss during maleimide hydrolysis.