Publications by authors named "Thomas S Corrigan"
Aza-peptide aldehydes and ketones are a new class of reversible protease inhibitors that are specific for the proteasome and clan CD cysteine proteases. We designed and synthesised aza-Leu derivatives that were specific for the chymotrypsin-like active site of the proteasome, aza-Asp derivatives that were effective inhibitors of caspases-3 and -6, and aza-Asn derivatives that inhibited and legumains. The crystal structure of caspase-3 in complex with our caspase-specific aza-peptide methyl ketone inhibitor with an aza-Asp residue at P1 revealed a covalent linkage between the inhibitor carbonyl carbon and the active site cysteinyl sulphur.
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- Organophosphorus (OP) nerve agents inhibit acetylcholinesterase (AChE) and can lead to an irreversible aging process, making traditional reactivators ineffective.
- Researchers synthesized a set of quinone methide precursors (QMPs) to potentially reverse this aging process, focusing on a lead compound called C8.
- C8 successfully restored a significant percentage of activity to aged AChE, with its effectiveness influenced by pH levels, indicating potential for treating OP nerve agent exposure.