Sun Mingjiang, Bai Lin, Liu David Q
GlaxoSmithKline Pharmaceutical R&D, King of Prussia, PA 19406, USA.
J Pharm Biomed Anal. 2009 Feb 20;49(2):529-33. doi: 10.1016/j.jpba.2008.11.009. Epub 2008 Nov 19.
In situ derivatization-headspace GC-MS methodology has been developed for the determination of hydrazine in drug substance at low ppm levels. This general method uses acetone or acetone-d(6) as the derivatization reagent. The resulting acetone azine or acetone azine-d(12) can then be analyzed by headspace GC-MS. The method gives excellent sensitivity with a limit of quantitation (LOQ) as low as 0.1ppm when the API (active pharmaceutical ingredient) samples are prepared at 10mg per headspace injection vial. The spike recoveries of hydrazine at the 1ppm level were between 79% and 117% in various APIs tested. The precisions (%RSD) of six preparations of the hydrazine standards at the concentration of 1ppm level were typically between 2.7 and 5.6%. A linear range of concentrations from 0.1 to 10ppm has been demonstrated with R(2)> or =0.999. This general method has been tested in a number of API matrices and successfully applied to the determination of hydrazine in support of API batch releases and process chemistry at GlaxoSmithKline.
已开发出原位衍生化-顶空气相色谱-质谱联用方法,用于测定原料药中低至百万分之几水平的肼。该通用方法使用丙酮或氘代丙酮(丙酮-d(6))作为衍生化试剂。然后可通过顶空气相色谱-质谱联用对生成的丙酮嗪或氘代丙酮嗪(丙酮嗪-d(12))进行分析。当在每个顶空进样瓶中制备10mg活性药物成分(API)样品时,该方法具有出色的灵敏度,定量限(LOQ)低至0.1ppm。在测试的各种原料药中,1ppm水平的肼加标回收率在79%至117%之间。1ppm浓度水平的六种肼标准品制剂的精密度(%RSD)通常在2.7%至5.6%之间。已证明浓度在0.1至10ppm之间呈线性范围,R(2)≥0.999。该通用方法已在多种原料药基质中进行了测试,并成功应用于葛兰素史克公司原料药批次放行和工艺化学中肼的测定。