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Lysine Covalent Antagonists of Melanoma Inhibitors of Apoptosis Protein

Parima Udompholkul, Carlo Baggio, Luca Gambini, Giulia Alboreggia, Maurizio Pellecchia

2021Journal of Medicinal Chemistry28 citationsDOIOpen Access PDF

Abstract

We have recently reported on Lys-covalent agents that, based on aryl-sulfonyl fluorides, were designed to target binding site Lys 311 in the X-linked inhibitor of apoptosis protein (XIAP). Similar to XIAP, melanoma-IAP (ML-IAP), a less well-characterized IAP family protein, also presents a lysine residue (Lys 135), which is in a position equivalent to that of Lys 311 of XIAP. On the contrary, two other members of the IAP family, namely, cellular-IAPs (cIAP1 and cIAP2), present a glutamic acid residue in that position. Hence, in the present work, we describe the derivation and characterization of the very first potent ML-IAP Lys-covalent inhibitor with cellular activity. The agent can be used as a pharmacological tool to further validate ML-IAP as a drug target and eventually for the development of ML-IAP-targeted therapeutics.

Topics & Concepts

XIAPInhibitor of apoptosisChemistryCovalent bondLysineResidue (chemistry)ApoptosisBiochemistryStructure–activity relationshipPharmacologyCancer researchStereochemistryCombinatorial chemistryAmino acidIn vitroProgrammed cell deathBiologyCaspaseOrganic chemistryClick Chemistry and ApplicationsUbiquitin and proteasome pathwaysProtein Degradation and Inhibitors
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