Tunable Thioesters as “Reduction” Responsive
Functionality for Traceless Reversible Protein PEGylation
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Abstract
Disulfide has been
the only widely used functionality to serve
as a reduction responsive trigger in drug delivery. We introduce thioester
as a novel thiol responsive chemistry for drug delivery, whose reactivity
can be conveniently modulated by choosing the appropriate steric environment
around the thioester. Compared with disulfides, thioesters are facile
to synthesize and have an order of magnitude broader kinetic tunability.
A novel traceless reversible protein PEGylation reagent is developed
based on thioester chemistry