Molecular Bidents with Two Electrophilic Warheads as a New Pharmacological Modality.

Publication Type:

Journal Article

Source:

ACS Cent Sci, Volume 10, Issue 6, p.1156-1166 (2024)

Abstract:

<p>A systematic strategy to develop dual-warhead inhibitors is introduced to circumvent the limitations of conventional covalent inhibitors such as vulnerability to mutations of the corresponding nucleophilic residue. Currently, all FDA-approved covalent small molecules feature one electrophile, leaving open a facile route to acquired resistance. We conducted a systematic analysis of human proteins in the protein data bank to reveal &sim;400 unique targets amendable to dual covalent inhibitors, which we term &quot;molecular bidents&quot;. We demonstrated this strategy by targeting two kinases: MKK7 and EGFR. The designed compounds, ZNL-8162 and ZNL-0056, are ATP-competitive inhibitors that form two covalent bonds with cysteines and retain potency against single cysteine mutants. Therefore, molecular bidents represent a new pharmacological modality with the potential for improved selectivity, potency, and drug resistance profile.</p>

PDB: 
8EME
Detector: 
EIGER
Beamline: 
24-ID-E