Department of Pharmaceutical Analysis, China Pharmaceutical University, Nanjing 211100, China.
Nanjing Clinical Tech. Laboratories Inc., Nanjing 211100, China.
J Pharm Biomed Anal. 2023 Sep 5;233:115498. doi: 10.1016/j.jpba.2023.115498. Epub 2023 Jun 1.
101BHG-D01 is a novel, long-acting and selective muscarinic receptor antagonist for the treatment of chronic obstructive pulmonary disease (COPD) and rhinorrhea in rhinitis. To support its clinical study, several liquid chromatography tandem mass spectrometry (LC-MS/MS) methods for the quantification of 101BHG-D01 and its main metabolite M6 in human plasma, urine and feces were developed. The plasma samples were prepared by protein precipitation, and the urine and fecal homogenate samples were pretreated by direct dilution, respectively. The chromatographic separation was performed on an Agilent InfinityLab Poroshell 120 C18 column with 0.1% formic acid and 10.0 mM ammonium acetate buffer solution in water and methanol as the mobile phase. The MS/MS analysis was performed by using multiple reaction monitoring (MRM) under a positive ion electrospray ionization mode. The methods were validated with regards to selectivity, linearity, lower limit of quantitation (LLOQ), accuracy and precision, matrix effect, extraction recovery, dilution integrity, batch size, carryover and stability. The calibration ranges were as follows: 1.00-800 pg/mL for 101BHG-D01 and 1.00-20.0 pg/mL for M6 in plasma; 0.0500-20.0 ng/mL for 101BHG-D01 and M6 in urine; 0.400-400 ng/mL for 101BHG-D01 and 0.100-100 ng/mL for M6 in feces. There was no endogenous or cross interference observed at the retention time of the analytes and internal standard in various biological matrices. Across these matrices, for the lower limit of quantitation quality control (LLOQ QC) samples, the intra- and inter-batch coefficients of variation were within 15.7%. For other QC samples, the intra- and inter-batch coefficients of variation were within 8.9%. The intra- and inter-batch accuracy deviations for all QC samples were within the range of - 6.2-12.0%. No significant matrix effect was observed from the matrices. The extraction recoveries of these methods at different concentrations were consistent and reproducible. The analytes were stable in different matrices under various storage conditions. The other bioanalytical parameters were also fully validated and met the criteria given in the FDA guidance. These methods were successfully applied to a clinical study in healthy Chinese subjects after a single dose administration of 101BHG-D01 inhalation aerosol. After inhalation, 101BHG-D01 was absorbed into plasma rapidly with the time to reach the maximum drug concentration (T) of 5 min and eliminated slowly with a half-life time about 30 h. The cumulative urinary and fecal excretion rates revealed 101BHG-D01 was mainly excreted in feces, rather than urine. The pharmacokinetic results of the study drug laid a foundation for its further clinical development.
101BHG-D01 是一种新型长效、选择性毒蕈碱受体拮抗剂,用于治疗慢性阻塞性肺疾病(COPD)和变应性鼻炎的鼻溢。为支持其临床研究,开发了几种用于定量测定人血浆、尿液和粪便中 101BHG-D01 及其主要代谢物 M6 的液相色谱-串联质谱(LC-MS/MS)方法。血浆样品通过蛋白沉淀法制备,尿液和粪便匀浆样品分别通过直接稀释预处理。采用 Agilent InfinityLab Poroshell 120 C18 柱进行色谱分离,流动相为 0.1%甲酸和 10.0 mM 乙酸铵缓冲液水溶液和甲醇。采用正离子电喷雾电离模式下的多重反应监测(MRM)进行 MS/MS 分析。方法经过选择性、线性、定量下限(LLOQ)、准确度和精密度、基质效应、提取回收率、稀释完整性、批大小、交叉污染和稳定性验证。校准范围如下:血浆中 101BHG-D01 为 1.00-800 pg/mL,M6 为 1.00-20.0 pg/mL;尿液中 101BHG-D01 和 M6 为 0.0500-20.0 ng/mL;粪便中 101BHG-D01 为 0.400-400 ng/mL,M6 为 0.100-100 ng/mL。在各种生物基质中,分析物和内标在保留时间上没有观察到内源性或交叉干扰。在这些基质中,对于定量下限质控(LLOQ QC)样品,批内和批间变异系数均在 15.7%以内。对于其他 QC 样品,批内和批间变异系数均在 8.9%以内。所有 QC 样品的批内和批间准确度偏差均在-6.2-12.0%范围内。基质无显著影响。不同浓度下这些方法的提取回收率一致且重现性好。在各种储存条件下,分析物在不同基质中稳定。其他生物分析参数也经过充分验证,符合 FDA 指南中的标准。这些方法成功应用于在中国健康受试者单次给予 101BHG-D01 吸入气雾剂后的临床研究。吸入后,101BHG-D01 迅速被吸收到血浆中,达峰时间(T)为 5 分钟,半衰期约为 30 小时,消除缓慢。尿和粪便累积排泄率表明 101BHG-D01 主要通过粪便排泄,而不是尿液。研究药物的药代动力学结果为其进一步的临床开发奠定了基础。
