Savaryn John P, Kikuchi Ryota, Qian Yuli, Ji Qin C, Jenkins Gary J, Bow Daniel A J, Mohamed Mohamed-Eslam F
Quantitative, Translational and ADME Sciences, AbbVie Inc., North Chicago, Illinois, USA.
Clinical Pharmacology, AbbVie Inc., North Chicago, Illinois, USA.
Clin Transl Sci. 2024 Dec;17(12):e70109. doi: 10.1111/cts.70109.
Recent reports suggest that plasma riboflavin may serve as a biomarker for BCRP inhibition in humans. However, the clinical data supporting this claim have been limited, with only two studies showing modest increases in riboflavin levels after administration of a BCRP inhibitor. We have recently demonstrated that co-administration of 375 mg once daily (q.d.) cedirogant, an in vitro BCRP inhibitor, significantly increased rosuvastatin (an OATP1B1/1B3 and BCRP substrate) exposures but did not change the levels of the OATP1B endogenous biomarker coproporphyrin-I, demonstrating that cedirogant is a clinical BCRP inhibitor. Samples from this same cedirogant clinical drug-drug interaction study were utilized to test the hypothesis that endogenous plasma riboflavin is a biomarker of BCRP inhibition. Plasma riboflavin levels in the absence of cedirogant ranged from 1 to 10 ng/mL across the 11 participants analyzed with minimal (<20%) intrasubject variability over a 24-hour interval. Contrary to expectations, 375 mg q.d. oral administration of cedirogant did not increase riboflavin levels. These data strongly suggest that endogenous plasma riboflavin is not a viable biomarker for BCRP inhibition in humans.
近期报告表明,血浆核黄素可能作为人体中乳腺癌耐药蛋白(BCRP)抑制作用的生物标志物。然而,支持这一说法的临床数据有限,仅有两项研究显示在给予BCRP抑制剂后核黄素水平有适度升高。我们最近证明,每日一次(q.d.)共同给予375毫克西地罗甘(一种体外BCRP抑制剂)可显著增加瑞舒伐他汀(一种有机阴离子转运多肽1B1/1B3和BCRP底物)的暴露量,但并未改变有机阴离子转运多肽1B内源性生物标志物粪卟啉-I的水平,这表明西地罗甘是一种临床BCRP抑制剂。来自同一西地罗甘临床药物相互作用研究的样本被用于检验内源性血浆核黄素是BCRP抑制作用生物标志物这一假设。在24小时间隔内,对11名参与者进行分析,未使用西地罗甘时血浆核黄素水平在1至10纳克/毫升之间,受试者内变异性最小(<20%)。与预期相反,每日口服375毫克西地罗甘并未提高核黄素水平。这些数据有力地表明,内源性血浆核黄素并非人体中BCRP抑制作用的可行生物标志物。
