AI Article Synopsis

  • Prolyl-tRNA synthetase (PRS) is a crucial enzyme for protein translation and a key target for malaria treatments.
  • Five newly developed ATP mimetics (L95, L96, L97, L35, and L36) show improved stability when interacting with L-proline, with L35 demonstrating the highest thermal stability and effectiveness similar to halofuginone.
  • L35 has a potent inhibitory effect (∼1.6 nM) against the asexual-blood-stage of the malaria parasite and exhibits a significant selectivity, meaning it targets the parasite more effectively than human proteins, showcasing potential for new drug development.

Article Abstract

The prolyl-tRNA synthetase (PRS) is an essential enzyme for protein translation and a validated target against malaria parasite. We describe five ATP mimetics (L95, L96, L97, L35, and L36) against PRS, exhibiting enhanced thermal stabilities in co-operativity with L-proline. L35 displays the highest thermal stability akin to halofuginone, an established inhibitor of PRS. Four compounds exhibit nanomolar inhibitory potency against PRS. L35 exhibits the highest potency of ∼1.6 nM against asexual-blood-stage (ABS) and ∼100-fold (effective concentration [EC]) selectivity for the parasite. The macromolecular structures of PRS with L95 and L97 in complex with L-pro reveal their binding modes and catalytic site malleability. Arg401 of PRS oscillates between two rotameric configurations when in complex with L95, whereas it is locked in one of the configurations due to the larger size of L97. Harnessing such specific and selective chemical features holds significant promise for designing potential inhibitors and expediting drug development efforts.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11298890PMC
http://dx.doi.org/10.1016/j.isci.2024.110049DOI Listing

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