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A highly sensitive LC-MS/MS method to determine novel Bruton's tyrosine kinase inhibitor spebrutinib: application to metabolic stability evaluation

机译:一种高度敏感的LC-MS / MS方法,用于确定新的Bruton的酪氨酸激酶抑制剂Spebrutinib:在代谢稳定性评估中的应用

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摘要

Spebrutinib (SBT) is a Bruton's tyrosine kinase inhibitor. SBT is currently in phase II and phase I clinical trials for the management of rheumatoid arthritis and chronic lymphocytic leukaemia, respectively. We developed and validated a liquid chromatography tandem mass spectrometry analytical method to quantify SBT and investigate its metabolic stability. SBT and the naquotinib as internal standard were isocratically eluted on a C18 column. The linearity of the developed method is 5–500 ng ml−1 (r2 ≥ 0.9999) in the human liver microsomes (HLMs) matrix. Good sensitivity was approved by the very low limit of detection (0.39 ng ml−1). Inter- and intra-assay accuracy values of −1.41 to 12.44 and precision values of 0.71% to 4.78%, were obtained. SBT was found to have an in vitro half-life (82.52 min) and intrinsic clearance (8.4 µl min−1 mg−1) as computed following its incubation with HLMs. The latter finding, hypothesize that SBT could be slowly excreted from the body unlike other related tyrosine kinase inhibitors. So, drug plasma level and kidney function should be monitored because of potential bioaccumulation. To the best of our knowledge, this is considered the first analytical method for SBT quantification using LC-MS/MS with application to metabolic stability evaluation.
机译:蜘蛛网(SBT)是一款Bruton的酪氨酸激酶抑制剂。 SBT目前处于II期和I期临床试验,用于管理类风湿性关节炎和慢性淋巴细胞白血病。我们开发并验证了液相色谱串联质谱分析方法,用于量化SBT并研究其代谢稳定性。 SBT和NaquoTinib作为内标在C18柱上进行了相当洗脱。开发方法的线性是人肝微粒体(HLMS)基质中5-500ng ml-1(R2≥0.9999)。通过极低的检测限(0.39 Ng ML-1)批准了良好的敏感性。获得-1.41至12.44的测定间精度值和0.71%至4.78%的精度值。发现SBT具有体外半衰期(82.52分钟)和固有间隙(8.4μlmin-1mg-1),如其与HLM一起孵育后计算的。后者发现,假设SBT可以与其他相关酪氨酸激酶抑制剂的身体缓慢排出。因此,由于潜在的生物累积,应监测药物血浆水平和肾功能。据我们所知,这被认为是使用LC-MS / MS应用于代谢稳定性评估的SBT定量的第一种分析方法。

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