International Journal of Molecular Sciences (Dec 2023)

Dissecting CYP1A2 Activation by Arylalkanoic Acid Prodrugs toward the Development of Anti-Inflammatory Agents

  • Maria Antonietta Occhiuzzi,
  • Giuseppina Ioele,
  • Michele De Luca,
  • Bruno Rizzuti,
  • Domenica Scordamaglia,
  • Rosamaria Lappano,
  • Marcello Maggiolini,
  • Antonio Garofalo,
  • Fedora Grande

DOI
https://doi.org/10.3390/ijms25010435
Journal volume & issue
Vol. 25, no. 1
p. 435

Abstract

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Arylalkane-derived prodrugs of arylacetic acids are a small group of substances that have long been known for their anti-inflammatory action. Despite their ease of synthesis and good potential for the development of new potent and safe anti-inflammatory agents, this group of substances has not received much attention from researchers so far. Therefore, representative arylalkane derivatives were investigated through molecular docking techniques to verify the possible hepatic activation mode toward active metabolites by CYP1A2. In this regard, arylalkanoic acid prodrugs were docked with a crystallographic structure of human CYP1A2, in which the enzyme is co-crystallized with the selective competitive inhibitor α-naphthoflavone BHF. Of note, all the examined compounds proved capable of interacting with the enzyme active site in a manner similar to Nabumetone, thus confirming that a productive metabolic transformation is feasible. On the basis of these findings, it is possible to argue that subtle differences in the way CYP1A2 accommodates the ligands depend on the fine details of their molecular structures. Overall, these data suggest that compounds simply formed by an aromatic moiety bearing an appropriate alkane-derived chain could lead to innovative anti-inflammatory agents.

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