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首页> 外文期刊>Journal of pharmaceutical sciences. >Quality-by-design: an integrated process analytical technology approach to determine the nucleation and growth mechanisms during a dynamic pharmaceutical coprecipitation process.
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Quality-by-design: an integrated process analytical technology approach to determine the nucleation and growth mechanisms during a dynamic pharmaceutical coprecipitation process.

机译:设计质量:一种集成的过程分析技术方法,用于确定动态药物共沉淀过程中的成核和生长机理。

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The objective of this study was to demonstrate the feasibility of using an integrated process analytical technology (PAT) approach to determine nucleation and growth mechanisms of a dynamic naproxen (drug)-Eudragit L100 (polymer) coprecipitation process. The influence of several thermodynamically important formulation and process variables (drug/polymer ratio, alcohol, and water usages) on coprecipitation process characteristics was investigated via real-time in situ focused beam reflectance measurement (FBRM) monitoring and near real-time particle vision microscopy measurement. The final products were characterized by near-infrared (NIR) spectroscopy and NIR chemical imaging microscopy. The coprecipitation nucleation induction time (t(ind) ) was measured by both FBRM trend statistics and process trajectory method, respectively. Furthermore, nucleation kinetics was evaluated based on t(ind) measurement and corresponding supersaturation ratio (S) estimated. It was found that plots of ln(t(ind) ) versus (ln(2) S)(-1) consist of two linear segments and are consistent with classical primary nucleation mechanisms. Apparently, the coprecipitation process is governed by heterogeneous primary nucleation mechanism at low S (14
机译:这项研究的目的是证明使用综合过程分析技术(PAT)方法确定动态萘普生(药物)-Eudragit L100(聚合物)共沉淀过程的成核和生长机理的可行性。通过实时原位聚焦光束反射率测量(FBRM)监测和近实时粒子视觉显微镜研究了几种热力学上重要的配方和工艺变量(药物/聚合物比,酒精和水的用量)对共沉淀工艺特性的影响。测量。最终产品通过近红外(NIR)光谱和NIR化学成像显微镜进行表征。共沉淀成核诱导时间(t(ind))分别通过FBRM趋势统计和过程轨迹方法进行测量。此外,基于t(ind)测量值评估了成核动力学,并估算了相应的过饱和比(S)。发现ln(t(ind))对(ln(2)S)(-1)的曲线由两个线性段组成,并且与经典的初级成核机制相一致。显然,共沉淀过程受低S(14

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