| Literature DB >> 33804018 |
Yusuke Kono1, Iichiro Kawahara2, Kohei Shinozaki2, Ikuo Nomura2, Honoka Marutani1, Akira Yamamoto2, Takuya Fujita1.
Abstract
For developing oral drugs, it is necessary to predict the oral absorption of new chemical entities accurately. However, it is difficult because of the involvement of efflux transporters, including P-glycoprotein (P-gp), in their absorption process. In this study, we conducted a comparative analysis on the inhibitory activities of seven P-gp inhibitors (cyclosporin A, GF120918, LY335979, XR9576, WK-X-34, VX-710, and OC144-093) to evaluate the effect of P-gp on drug absorption. GF120918, LY335979, and XR9576 significantly decreased the basal-to-apical transport of paclitaxel, a P-gp substrate, across Caco-2 cell monolayers. GF120918 also inhibited the basal-to-apical transport of mitoxantrone, a breast cancer resistance protein (BCRP) substrate, in Caco-2 cells, whereas LY335979 hardly affected the mitoxantrone transport. In addition, the absorption rate of paclitaxel after oral administration in wild-type mice was significantly increased by pretreatment with LY335979, and it was similar to that in mdr1a/1b knockout mice. Moreover, the absorption rate of topotecan, a BCRP substrate, in wild-type mice pretreated with LY335979 was similar to that in mdr1a/1b knockout mice but significantly lower than that in bcrp knockout mice. These results indicate that LY335979 has a selective inhibitory activity for P-gp, and would be useful for evaluating the contribution of P-gp to drug absorption.Entities:
Keywords: LY335979; P-glycoprotein; WK-X-34; breast cancer resistance protein; intestinal absorption
Year: 2021 PMID: 33804018 PMCID: PMC7999658 DOI: 10.3390/pharmaceutics13030388
Source DB: PubMed Journal: Pharmaceutics ISSN: 1999-4923 Impact factor: 6.321