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Conjugation of phosphonoacetic acid to nucleobase promotes a mechanism-based inhibition

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Date
2018
Author
Mikalkėnas, Algirdas
Ravoitytė, Bazilė
Tauraitė, Daiva
Servienė, Elena
Meškys, Rolandas
Serva, Saulius
Metadata
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Abstract
Small molecule inhibitors have a powerful blocking action on viral polymerases. The bioavailability of the inhibitor, nevertheless, often raise a significant selectivity constraint and may substantially limit the efficacy of therapy. Phosphonoacetic acid has long been known to possess a restricted potential to block DNA biosynthesis. In order to achieve a better affinity, this compound has been linked with natural nucleotide at different positions. The structural context of the resulted conjugates has been found to be crucial for the acquisition by DNA polymerases. We show that nucleobase-conjugated phosphonoacetic acid is being accepted, but this alters the processivity of DNA polymerases. The data presented here not only provide a mechanistic rationale for a switch in the mode of DNA synthesis, but also highlight the nucleobase-targeted nucleotide functionalization as a route for enhancing the specificity of small molecule inhibitors.
Issue date (year)
2018
URI
https://etalpykla.vilniustech.lt/handle/123456789/119735
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  • Straipsniai Web of Science ir/ar Scopus referuojamuose leidiniuose / Articles in Web of Science and/or Scopus indexed sources [7946]

 

 

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