Pós-Graduação em Engenharia e Ciência de Materiais, Instituto de Ciência e Tecnologia (ICT), Universidade Federal de São Paulo (UNIFESP), São Paulo, Brasil.
Pós-Graduação em Engenharia e Ciência de Materiais, Instituto de Ciência e Tecnologia (ICT), Universidade Federal de São Paulo (UNIFESP), São Paulo, Brasil; Laboratório de Micro e Nanotecnologia, Instituto de Tecnologia em Fármacos /Farmanguinhos (FIOCRUZ), Rio de Janeiro, Brasil.
J Pharm Biomed Anal. 2024 May 15;242:116038. doi: 10.1016/j.jpba.2024.116038. Epub 2024 Feb 15.
In the pharmaceutical industry, the unexpected appearance of crystalline forms could impact the therapeutic efficacy of an Active Pharmaceutical Ingredient (API). For quality control, a thorough qualitative and quantitative monitoring of pharmaceutical solid forms is essential to ensure the detection and the quantification of crystalline forms, wither different or with the same chemical composition (polymorphs) at a low detection level. The purpose of this paper was to review and highlight the importance of choosing adequate solid-state techniques for detection and quantification APIs that present polymorphism - based on limits of detection (LOD) and quantification (LOQ), pharmacopeias specifications, international guidelines and studies reported in the literature. To this study, the powder X-ray diffraction (PXRD), differential scanning calorimetry (DSC), Infrared and Raman spectroscopies and solid-state nuclear magnetic resonance (NMR) were the solid-state techniques analyzed. Additionally, the Argentine, Brazilian, British, European, International, Japanese, Mexican and the United States of America pharmacopeias were reviewed. Based on the analysis performed, the advantages and disadvantages of these techniques, as well as the LOD and LOQ values of APIs were reported. In comparison to these solid-state techniques, reference material used for identification analyses should be previously identified with the corresponding polymorph. Without this previous procedure, the patterns, the spectra, and DSC curves of the reference material can only be used to confirm the mixture of solid forms, not being able to specify which polymorphs are contained in the sample. A major advantage of PXRD is the use of the calculated diffraction patterns obtained from the Crystallographic Information Frameworks (CIFs) files which could be used as a reference pattern without any other information, assistance technique, or physical standards. Regarding the quantification aspect, different pharmacopeias suggest various methods such as the PXRD combining with Rietveld method, which can be used to obtain lower LOD values for minority phases in the mixture of different substances without the need for a calibration curve. Raman spectroscopy can detect polymorphs in small particles and solid-state NMR spectroscopy is a powerful technique for quantification not only crystalline but also crystalline-amorphous mixtures. Finally, this review intends to be a useful tool to control, with efficiency and accuracy, the polymorphism of APIs in pharmaceutical compounds.
在制药行业中,意外出现的晶体形式可能会影响活性药物成分 (API) 的治疗效果。为了进行质量控制,彻底监测药物固体形式的定性和定量分析对于确保检测和量化不同或具有相同化学成分(多晶型物)的晶体形式至关重要,即使在低检测水平下也是如此。本文的目的是回顾并强调选择适当的固态技术来检测和量化具有多晶型性的 API 的重要性——基于检测限 (LOD) 和定量限 (LOQ)、药典规范、国际指南和文献中报道的研究。在这项研究中,粉末 X 射线衍射 (PXRD)、差示扫描量热法 (DSC)、红外和拉曼光谱以及固态核磁共振 (NMR) 被分析为固态技术。此外,还审查了阿根廷、巴西、英国、欧洲、国际、日本、墨西哥和美国的药典。根据进行的分析,报告了这些技术的优缺点,以及 API 的 LOD 和 LOQ 值。与这些固态技术相比,用于鉴定分析的参考材料应事先与相应的多晶型物进行鉴定。如果没有这个前期步骤,参考材料的图谱、光谱和 DSC 曲线只能用于确认固体形式的混合物,而无法指定样品中包含哪些多晶型物。PXRD 的一个主要优点是使用从晶体学信息框架 (CIFs) 文件获得的计算衍射图案,可以在没有任何其他信息、辅助技术或物理标准的情况下用作参考图案。关于定量方面,不同的药典建议了各种方法,例如 PXRD 与 Rietveld 方法相结合,可以用于在不使用校准曲线的情况下,获得混合物中少数相的更低 LOD 值。拉曼光谱可以检测小颗粒中的多晶型物,固态核磁共振光谱是一种强大的技术,不仅可以用于定量结晶相,还可以用于定量结晶-非晶混合物。最后,本综述旨在成为一种有用的工具,用于有效地、准确地控制药物化合物中 API 的多晶型性。
