AI Article Synopsis

  • - Aprepitant (APT) is a drug that helps prevent nausea and vomiting caused by chemotherapy, including the drug imatinib (IMA), and this study looked at how APT affects the levels of IMA in rats.
  • - After giving rats APT for three days, the levels of IMA in the blood were lower regardless of how it was administered (oral or intravenous), while the metabolite N-desmethyl imatinib (N-D IMA) levels stayed roughly the same.
  • - The study found that APT increased the clearance of IMA from the body and decreased its bioavailability significantly, suggesting that APT interacts with IMA through the enhancement of certain proteins (P-gp and CYP

Article Abstract

Aprepitant (APT), an antiemetic drug belonging to the class of substance P antagonists is efficiently used in both acute and delayed chemotherapy-induced nausea and vomiting. Nausea and vomiting induced by imatinib (IMA) as a chemotherapeutic drug could be reduced by APT. This study investigated the effect of APT on the pharmacokinetics of IMA and its major metabolite N-desmethyl imatinib (N-D IMA) in rats and the mechanism of this drug-drug interaction. The results indicated that after 3 days of pretreatment with APT (10 mg/kg), the blood concentration of IMA was decreased in both of oral and intravenous routes of IMA administration compared to vehicle treated rats, whereas the blood concentration of N-D IMA was not significantly changed. The total clearance (CL/F) of oral and intravenous given IMA was increased by 1.41 and 1.32-fold, and the bioavailability was greatly decreased about 30.43% and 24.40% respectively. At this time, the P-gp and the hepatic CYP3A1 were increased at both the mRNA and protein levels. These results demonstrated that ingestion of APT will decrease the bioavailability of IMA to a significant extent in rats and the drug-drug interaction between APT and IMA appears to be due to modulation of P-gp and CYP3A1.

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Source
http://dx.doi.org/10.1691/ph.2018.7335DOI Listing

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