AI Article Synopsis

  • ON 01210.Na (Ex-RAD) is a new compound created by Onconova Therapeutics as a radioprotectant, and research aimed to analyze its behavior in rat liver and the influence of ethacrynic acid (EA) on its pharmacokinetics.
  • The study found that ON 01210.Na had strong binding properties in liver perfusate, but this binding decreased when EA was present, along with a notable drop in hepatic clearance as doses increased.
  • Results indicated that EA significantly hinders the metabolism of ON 01210.Na to its GSH conjugate, leading to lower clearance rates and prolonged presence in the body, positioning EA as a potential enhancer for the drug's effectiveness.

Article Abstract

ON 01210.Na (Ex-RAD) is a novel benzyl styryl sulfone analog, developed as a radioprotectant by Onconova Therapeutics Inc. The objectives of this research were to evaluate the hepatobiliary disposition of ON 01210.Na in the isolated perfused rat liver (IPRL) and to determine the effect of coadministration of ethacrynic acid (EA) on the pharmacokinetic profile of ON 01210.Na. EA acid was used as a prototypical inhibitor of glutathione-S-transferase inhibitor. ON 01210.Na was highly bound in IPRL perfusate proteins, and binding was significantly lower in the presence of EA. Dose-escalation studies (bolus dose, target concentrations 10-250 μg/mL) showed that ON 01210.Na followed nonlinear pharmacokinetics with hepatic clearance decreasing from 3.14 to 1.99 mL/min with increasing dose. ON 01210.Na underwent extensive metabolic degradation to its glutathione (GSH) adduct in liver. The GSH metabolite was mainly excreted into the bile. Coadministration of EA (1 mM) significantly inhibited the conversion of ON 01210.Na to its GSH conjugate, resulting in decreased clearance (approx. fivefold lower), and prolonged elimination from the perfusate. These preclinical studies suggest that EA is a potential pharmacoenhancer that can reduce the metabolism of ON 01210.Na in vivo, thereby increasing drug exposure and boosting radioprotective activity.

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http://dx.doi.org/10.1002/jps.23391DOI Listing

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