Drug interaction of ningetinib and gefitinib involving CYP1A1 and efflux transporters in non-small cell lung cancer patients.

Lu Liu Qian WangCen XieNing XiZitao GuoMing LiXiangyu HouNingjie Xie Mingming Sun Jing Li Xiaoyan Chen

Published in: British journal of clinical pharmacology (2020)

The high plasma exposure of M1 in patients was attributed to the inhibition of M1 efflux by ningetinib and its low tissue affinity. When co-administered, gefitinib inhibited the formation of M1, but due to the low metabolic yield of M1 in vivo, the pharmacokinetics of ningetinib was not influenced. Inhibition of CYP1A1 may increase the concentration of ningetinib in target tissues, and the long-term safety and efficacy of ningetinib combined with gefitinib should be evaluated.

Keyphrases

small cell lung cancer
epidermal growth factor receptor
end stage renal disease
ejection fraction
newly diagnosed
chronic kidney disease
gene expression
prognostic factors
single cell
cell therapy
patient reported outcomes
tyrosine kinase
drug induced