Publications by authors named "Oksana P Kovalenko"

Effective treatment of tuberculosis is challenged by the rapid development of () multidrug resistance that presumably could be overcome with novel multi-target drugs. Aminoacyl-tRNA synthetases (AARSs) are an essential part of protein biosynthesis machinery and attractive targets for drug discovery. Here, we experimentally verify a hypothesis of simultaneous targeting of structurally related AARSs by a single inhibitor.

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Mycobacterium tuberculosis infection remains a major cause of global morbidity and mortality due to the increase of antibiotics resistance. Dual/multi-target drug discovery is a promising approach to overcome bacterial resistance. In this study, we built ligand-based pharmacophore models and performed pharmacophore screening in order to identify hit compounds targeting simultaneously two enzymes-M.

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Article Synopsis
  • d-aminoacyl-tRNA-deacylase (DTD) prevents incorrect incorporation of d-amino acids into proteins by breaking the bond between misattached amino acids and tRNAs during translation.
  • Recent biochemical and computational studies revealed a new substrate-assisted mechanism for the hydrolysis of d-Tyr-tRNA by DTD, highlighting the role of certain functional elements in the reaction.
  • Key findings indicate that the d-Tyr amino group acts as a general base in the hydrolysis process, with specific amino acid residues of the enzyme aiding in substrate coordination, thus enhancing understanding of translation fidelity.
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Aminoacyl-tRNA-synthetases are crucial enzymes for initiation step of translation. Possessing editing activity, they protect living cells from misincorporation of non-cognate and non-proteinogenic amino acids into proteins. Tyrosyl-tRNA synthetase (TyrRS) does not have such editing properties, but it shares weak stereospecificity in recognition of d-/l-tyrosine (Tyr).

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The increase of antibiotic resistance amongst Mycobacterium tuberculosis strains has become one of the most pressing problems of modern medicine. Therefore, the search of antibiotics against M. tuberculosis with novel mechanisms of action is very important.

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Tuberculosis is a serious infectious disease caused by human pathogen bacteria Mycobacterium tuberculosis. Bacterial drug resistance is a very significant medical problem nowadays and development of novel antibiotics with different mechanisms of action is an important goal of modern medical science. Leucyl-tRNA synthetase (LeuRS) has been recently clinically validated as antimicrobial target.

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