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一种连续生产药品制药过程的停留时间分布(RTD)模型控制策略的开发与应用

Development and Use of a Residence Time Distribution (RTD) Model Control Strategy for a Continuous Manufacturing Drug Product Pharmaceutical Process.

作者信息

Hurley Samantha, Tantuccio Anthony, Escotet-Espinoza Manuel Sebastian, Flamm Matthew, Metzger Matthew

机构信息

Pharmaceutical Commercialization Technology, Merck & Co., Inc., West Point, PA 19486, USA.

Pharmaceutical Sciences, Merck & Co., Inc., Rahway, NJ 07065, USA.

出版信息

Pharmaceutics. 2022 Feb 3;14(2):355. doi: 10.3390/pharmaceutics14020355.

Abstract

Residence-time-distribution (RTD)-based models are key to understanding the mixing dynamics of continuous manufacturing systems. Such models can allow for material traceability throughout the process and can provide the ability for removal of non-conforming material from the finished product. These models have been implemented in continuous pharmaceutical manufacturing mainly for monitoring purposes, not as an integral part of the control strategy and in-process specifications. This paper discusses the steps taken to develop an RTD model design space and how the model was statistically incorporated into the product's control strategy. To develop the model, experiments were conducted at a range of blender impeller speeds and total system mass flow rates. RTD parameters were optimized for each condition tested using a tank-in-series-type model with a delay. Using the experimental RTD parameters, an equation was derived relating the mean residence time to the operating conditions (i.e., blender impeller speed and mass flow rate). The RTD parameters were used in combination with real-time upstream process data to predict downstream API concentration, where these predictions allowed validation across the entire operating range of the process by comparison to measured tablet assay. The standard in-process control limits for the product were statistically tightened using the validation acceptance criteria. Ultimately, this model and strategy were accepted by regulatory authorities.

摘要

基于停留时间分布(RTD)的模型是理解连续制造系统混合动力学的关键。此类模型能够实现整个过程中的物料可追溯性,并具备从成品中去除不合格物料的能力。这些模型在连续制药生产中主要用于监测目的,而非作为控制策略和过程规范的一个组成部分。本文讨论了开发RTD模型设计空间所采取的步骤,以及该模型如何在统计上纳入产品的控制策略。为了开发该模型,在一系列搅拌器叶轮速度和系统总质量流率下进行了实验。使用带有延迟的串联罐式模型针对每个测试条件优化RTD参数。利用实验得到的RTD参数,推导出一个将平均停留时间与操作条件(即搅拌器叶轮速度和质量流率)相关联的方程。RTD参数与实时上游过程数据相结合,用于预测下游活性药物成分(API)浓度,通过与实测片剂分析结果进行比较,这些预测能够在整个过程操作范围内进行验证。使用验证验收标准在统计上收紧了产品的标准过程控制限度。最终,该模型和策略获得了监管机构的认可。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d4d0/8874656/bcf74eed44c9/pharmaceutics-14-00355-g001.jpg

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