Michael J. Shapiro scite author profile

Interest in drugs that covalently modify their target is driven by the desire for enhanced efficacy that can result from the silencing of enzymatic activity until protein resynthesis can occur, along with the potential for increased selectivity by targeting uniquely positioned nucleophilic residues in the protein. However, covalent approaches carry additional risk for toxicities or hypersensitivity reactions that can result from covalent modification of unintended targets. Here we describe methods for measuring the reactivity of covalent reactive groups (CRGs) with a biologically relevant nucleophile, glutathione (GSH), along with kinetic data for a broad array of electrophiles. We also describe a computational method for predicting electrophilic reactivity, which taken together can be applied to the prospective design of thiol-reactive covalent inhibitors.

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International Classification of Retinopathy of Prematurity, Third Edition

Chiang

et al. 2021

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1,3- diastereoselective reduction of β-hydroxyketones utilizing alkoxydialkylboranes

Chen¹,

Hardtmann²,

Prasad³

et al. 1987

Tetrahedron Letters

437

203

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