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Scale-up from batch to flow-through wet milling process for injectable depot formulation

机译:对于可注射的储库配方,从批量扩大到流通湿磨工艺

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摘要

Injectable depot formulations are aimed at providing long-term sustained release of a drug into systemic circulation, thus reducing plasma level fluctuations and improving patient compliance. The particle size distribution of the formulation in the form of suspension is a key parameter that controls the release rate. In this work, the process of wet stirred media milling (ball milling) of a poorly water-soluble substance has been investigated with two main aims: (i) to determine the parametric sensitivity of milling kinetics; and (ii) to develop scale-up methodology for process transfer from batch to flow-through arrangement. Ball milling experiments were performed in two types of ball mills, a batch mill with a 30ml maximum working volume, and a flow-through mill with a 250ml maximum working volume. Milling parameters were investigated in detail by methodologies of QbD to map the parametric space. Specifically, the effects of ball size, ball fill level, and rpm on the particle breakage kinetics were systematically investigated at both mills, with an additional parameter (flow-rate) in the case of the flow-through mill. The breakage rate was found to follow power-law kinetics with respect to dimensionless time, with an asymptotic d50 particle size in the range of 200-300nm. In the case of the flow-through mill, the number of theoretical passes through the mill was found to be an important scale-up parameter.
机译:可注射的储库制剂旨在提供药物向体循环的长期持续释放,从而减少血浆水平的波动并改善患者的依从性。悬浮液形式的制剂的粒度分布是控制释放速率的关键参数。在这项工作中,研究了水溶性差的物质的湿式搅拌介质研磨(球磨)的过程,其主要目的有两个:(i)确定研磨动力学的参数敏感性; (ii)开发扩大规模的方法,以实现从批处理到流通安排的过程转移。球磨实验是在两种类型的球磨机中进行的:最大工作体积为30ml的间歇式研磨机和最大工作体积为250ml的流通式研磨机。通过QbD方法对铣削参数进行了详细研究,以绘制参数空间。具体而言,在两台磨机上系统地研究了球尺寸,球填充量和rpm对颗粒破碎动力学的影响,对于流通式磨机,还附加了参数(流速)。发现破损率遵循关于无量纲时间的幂律动力学,渐进d50粒度在200-300nm的范围内。对于流通式磨粉机,理论上通过磨粉机的次数是一个重要的放大参数。

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