首页> 外文期刊>Journal of Pharmaceutical and Biomedical Analysis: An International Journal on All Drug-Related Topics in Pharmaceutical, Biomedical and Clinical Analysis >Raman spectroscopy as a process analytical technology (PAT) tool for the in-line monitoring and understanding of a powder blending process.
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Raman spectroscopy as a process analytical technology (PAT) tool for the in-line monitoring and understanding of a powder blending process.

机译:拉曼光谱法是一种过程分析技术(PAT)工具,用于在线监控和了解粉末混合过程。

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The aim of this study is to propose a strategy to implement a PAT system in the blending step of pharmaceutical production processes. It was examined whether Raman spectroscopy can be used as PAT tool for the in-line and real-time endpoint monitoring and understanding of a powder blending process. A screening design was used to identify and understand the significant effects of two process variables (blending speed and loading of the blender) and of a formulation variable (concentration of active pharmaceutical ingredient (API): diltiazem hydrochloride) upon the required blending time (response variable). Interactions between the variables were investigated as well. A Soft Independent Modelling of Class Analogy (SIMCA) model was developed to determine the homogeneity of the blends in-line and real-time using Raman spectroscopy in combination with a fiber optical immersion probe. One blending experiment was monitored using Raman and NIR spectroscopy simultaneously. This was done to verify whether two independent monitoring tools can confirm each other's endpoint conclusions. The analysis of the experimental design results showed that the measured endpoints were excessively rounded due to the large measurement intervals relative to the first blending times. This resulted in effects and critical effects which cannot be interpreted properly. To be able to study the effects properly, the ratio between the blending times and the measurement intervals should be sufficiently high. In this study, it anyway was demonstrated that Raman spectroscopy is a suitable PAT tool for the endpoint control of a powder blending process. Raman spectroscopy not only allowed in-line and real-time monitoring of the blend homogeneity, but also helped to understand the process better in combination with experimental design. Furthermore, the correctness of the Raman endpoint conclusions was demonstrated for one process by using a second independent endpoint monitoring tool (NIR spectroscopy). Hence, the use of two independent techniques for the control of one response variable not only means a mutual confirmation of both methods, but also provides a higher certainty in the determined endpoint.
机译:这项研究的目的是提出一种在制药生产过程的混合步骤中实施PAT系统的策略。检查了拉曼光谱是否可用作在线和实时终点监测以及了解粉末混合过程的PAT工具。筛选设计用于识别和了解两个过程变量(混合速度和搅拌器的装载量)和配方变量(活性药物成分(API)的浓度:盐酸地尔硫卓)对所需混合时间(响应)的重大影响。变量)。还研究了变量之间的相互作用。开发了软独立类比建模(SIMCA)模型,以结合拉曼光谱法和光纤浸没探针在线和实时确定共混物的均匀性。同时使用拉曼光谱和近红外光谱监测一个混合实验。这样做是为了验证两个独立的监视工具是否可以确认彼此的端点结论。对实验设计结果的分析表明,由于相对于第一次混合时间的测量间隔较大,因此测量的端点过于舍入。这导致无法正确解释的影响和严重影响。为了能够正确地研究效果,混合时间和测量间隔之间的比率应足够高。在这项研究中,无论如何证明拉曼光谱是用于粉末混合过程终点控制的合适PAT工具。拉曼光谱不仅可以在线和实时监控共混物的均匀性,而且结合实验设计有助于更好地了解该过程。此外,通过使用第二个独立的终点监测工具(NIR光谱),证明了拉曼终点结论在一种方法中的正确性。因此,使用两种独立的技术来控制一个响应变量不仅意味着两种方法的相互确认,而且在确定的端点上具有更高的确定性。

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