Department of Chemistry, Brandeis University, Waltham, Massachusetts 02453, United States.
Pharmaceutical Sciences, Merck & Co., Inc., Kenilworth, New Jersey 07033, United States.
Mol Pharm. 2020 Sep 8;17(9):3567-3580. doi: 10.1021/acs.molpharmaceut.0c00592. Epub 2020 Aug 19.
Molecular miscibility and homogeneity of amorphous solid dispersions (ASDs) are critical attributes that impact physicochemical stability, bioavailability, and processability. Observation of a single glass transition is utilized as a criterion for good mixing of drug substance and polymeric components but can be misleading and cannot quantitatively analyze the domain size at high resolution. While imaging techniques, on the other hand, can characterize phase separation on the particle surface at the nanometer scale, they often require customized sample preparation and handling. Moreover, a mixed system is not necessarily homogeneous. Compared to the numerous studies that have evaluated the mixing of drug substance and polymer in ASDs, inhomogeneity in the phase compositions has remained significantly underexplored. To overcome the analytical challenge, we have developed a H spin diffusion NMR technique to quantify molecular mixing of bulk ASDs at sub-100 nm resolution. It combines relaxation filtering ( and ) that leaves the active pharmaceutical ingredient (API) as the main source of H magnetization at the start of spin diffusion to the polymer matrix. A spray-dried nifedipine-poly(vinylpyrrolidone) (Nif-PVP) ASD at a 5 wt % drug loading was a homogeneous reference system that exhibited equilibration of magnetization transfer from API to polymer within a short spin diffusion time of ∼3 ms. While fast initial magnetization transfer proving mixing on the 1 nm scale was also observed in Nif-PVP ASDs prepared by hot-melt extrusion (HME) at 186 °C at a 40 wt % drug loading, incomplete equilibration of peak intensities documented inhomogeneity on the ≥30 nm scale. The nonuniformity was confirmed by the partial inversion of the Nif magnetization in the filter that resulted in an even more pronounced deviation from equilibration and by H-C heteronuclear correlation (HETCOR) NMR. It is consistent with the observed differential H spin-lattice relaxation of Nif and PVP as well as a domain structure on the 20 nm scale observed in atomic force microscopy (AFM) images. The incomplete equilibration and differential relaxation were consistently reproduced in a model of two mixed phases of different compositions, e.g., 40 wt % of the ASD with a 15 wt % drug loading and the remaining 60 wt % with a 56 wt % drug loading. Hot-melt extrusion produced more inhomogeneous samples than spray drying for the samples examined in our study. To the best of our knowledge, this spin diffusion NMR method provides currently the highest-resolution quantification of inhomogeneous molecular mixing and phase composition in bulk samples of pharmaceutical dispersions produced with equipment, procedures, and drug loadings that are relevant to industrial drug development.
无定形固体分散体 (ASD) 的分子混溶性和均一性是影响物理化学稳定性、生物利用度和可加工性的关键属性。观察到单一玻璃化转变被用作药物物质和聚合物成分混合良好的标准,但可能具有误导性,并且不能定量分析高分辨率下的域尺寸。另一方面,成像技术可以在纳米尺度上表征颗粒表面的相分离,但它们通常需要定制的样品制备和处理。此外,混合系统不一定是均匀的。与评估 ASD 中药物物质和聚合物混合的众多研究相比,相组成的不均匀性仍然严重未被探索。为了克服分析挑战,我们开发了一种 H 自旋扩散 NMR 技术,以在亚 100nm 分辨率下定量测量大块 ASD 的分子混合。它结合了弛豫过滤( 和 ),该过滤在自旋扩散开始时将活性药物成分(API)作为聚合物基质中 H 磁化的主要来源。在 5wt%药物负载下喷雾干燥的硝苯地平-聚乙烯吡咯烷酮(Nif-PVP) ASD 是一个均匀的参考系统,在约 3ms 的短自旋扩散时间内显示出 API 到聚合物的磁化转移平衡。虽然在 186°C 下以 40wt%药物负载通过热熔挤出(HME)制备的 Nif-PVP ASD 中也观察到快速的初始磁化转移,证明了 1nm 尺度上的混合,但在 ≥30nm 尺度上记录的峰强度不完全平衡表明存在不均匀性。非均匀性通过 Nif 磁化在过滤器中的部分反转得到证实,这导致与平衡的更明显偏差,并通过 H-C 异核相关(HETCOR)NMR 得到证实。它与观察到的硝苯地平的差异 H 自旋晶格弛豫以及原子力显微镜 (AFM) 图像中观察到的 20nm 尺度上的畴结构一致。在两个混合相具有不同组成的模型中,例如,40wt%的 ASD 具有 15wt%的药物负载,其余 60wt%的 ASD 具有 56wt%的药物负载,观察到的不完全平衡和差异弛豫可以得到一致再现。与我们研究中检查的样品相比,热熔挤出产生的样品比喷雾干燥更不均匀。据我们所知,这种自旋扩散 NMR 方法目前提供了在与工业药物开发相关的设备、程序和药物负载下生产的药物分散体的大块样品中不均匀分子混合和相组成的最高分辨率定量。
