Ruggenthaler M, Grass J, Schuh W, Huber C G, Reischl R J
SANDOZ GmbH, Biochemiestraße 10, A-6250 Kundl/Tirol, Austria; Department of Molecular Biology, Division of Chemistry and Bioanalytics, University of Salzburg, Hellbrunner Straße 34, A-5020 Salzburg, Austria.
SANDOZ GmbH, Biochemiestraße 10, A-6250 Kundl/Tirol, Austria.
J Pharm Biomed Anal. 2017 Sep 5;143:147-158. doi: 10.1016/j.jpba.2017.05.039. Epub 2017 May 30.
For the first time, a comprehensive investigation of the impurity profile of the synthetic thyroid API (active pharmaceutical ingredient) liothyronine sodium (LTNa) was performed by using reversed phase HPLC and advanced structural elucidation techniques including high resolution tandem mass spectrometry (HRMS/MS) and on-line hydrogen-deuterium (H/D) exchange. Overall, 39 compounds were characterized and 25 of these related substances were previously unknown to literature. The impurity classification system recently developed for the closely related API levothyroxine sodium (LTNa) could be applied to the newly characterized liothyronine sodium impurities resulting in a wholistic thyroid API impurity classification system. Furthermore, the mass-spectrometric CID-fragmentation of specific related substances was discussed and rationalized by detailed fragmentation pathways. Moreover, the UV/Vis absorption characteristics of the API and selected impurities were investigated to corroborate chemical structure assignments derived from MS data.
首次采用反相高效液相色谱法以及包括高分辨率串联质谱法(HRMS/MS)和在线氢-氘(H/D)交换在内的先进结构解析技术,对合成甲状腺活性药物成分(API)左甲状腺素钠(LTNa)的杂质概况进行了全面研究。总体而言,共鉴定出39种化合物,其中25种相关物质在文献中尚无报道。最近为密切相关的API左甲状腺素钠(LTNa)开发的杂质分类系统可应用于新鉴定出的左甲状腺素钠杂质,从而形成一个完整的甲状腺API杂质分类系统。此外,还通过详细的裂解途径对特定相关物质的质谱CID裂解进行了讨论并给出了合理解释。此外,还研究了该API和选定杂质的紫外/可见吸收特性,以证实从质谱数据得出的化学结构归属。
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