通过直接压制连续生产口服固体制剂的质量控制方法

Qinglin Su, Sudarshan Ganesh, Dan Bao Le Vo, Anushaa Nukala, Yasasvi Bommireddy, Marcial Gonzalez, Gintaras V Reklaitis, Zoltan K Nagy
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引用次数: 0

摘要

制药业一直在向连续生产模式转变,在这种模式下,实时产品质量保证的新方法得到了研究。最近,一种名为 "质量控制(QbC)"的新观点被提出来,作为一种重要的扩展和补充方法,以实现全面的质量控制(QbD)。在本研究中,针对连续直接压制工艺中的商业规模压片机演示了 QbC 方法。首先,在 QbD 指导下,使用试验规模压片机 Natoli BLP-16 对模型配方的可压缩性进行了必要的了解。其次,根据对商用压片机 Natoli NP-400 的了解,采用数据调节策略调节片剂重量测量。此外,还考虑了参数估计,以监测和更新材料属性差异。第三,针对商业规模压片机的快速工艺动态,设计了一种分级式三级控制策略。该策略包括 0 级内置机器控制,用于片剂重量、预压缩力、主压缩力和生产率控制的 1 级解耦比例积分微分(PID)控制回路,以及 2 级传感器测量数据调节。在旋转压片机上展示的有效、可靠的性能证实,基于产品和工艺知识以及先进的基于模型的技术的质量控制方法可以确保药品连续生产的稳健性和效率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Quality-by-Control Approach in Pharmaceutical Continuous Manufacturing of Oral Solid Dosage via Direct Compaction.

A Quality-by-Control Approach in Pharmaceutical Continuous Manufacturing of Oral Solid Dosage via Direct Compaction.

A Quality-by-Control Approach in Pharmaceutical Continuous Manufacturing of Oral Solid Dosage via Direct Compaction.

A Quality-by-Control Approach in Pharmaceutical Continuous Manufacturing of Oral Solid Dosage via Direct Compaction.

The pharmaceutical industry has been undergoing a paradigm shift towards continuous manufacturing, under which novel approaches to real-time product quality assurance have been investigated. A new perspective, entitled Quality-by-Control (QbC), has recently been proposed as an important extension and complementary approach to enable comprehensive Quality-by-Design (QbD) implementation. In this study, a QbC approach was demonstrated for a commercial scale tablet press in a continuous direct compaction process. First, the necessary understanding of the compressibility of a model formulation was obtained under QbD guidance using a pilot scale tablet press, Natoli BLP-16. Second, a data reconciliation strategy was used to reconcile the tablet weight measurement based on this understanding on a commercial scale tablet press, Natoli NP-400. Parameter estimation to monitor and update the material property variance was also considered. Third, a hierarchical three-level control strategy, which addressed the fast process dynamics of the commercial scale tablet press was designed. The strategy consisted of the Level 0 built-in machine control, Level 1 decoupled Proportional Integral Derivative (PID) control loops for tablet weight, pre-compression force, main compression force, and production rate control, and Level 2 data reconciliation of sensor measurements. The effective and reliable performance, which could be demonstrated on the rotary tablet press, confirmed that a QbC approach, based on product and process knowledge and advanced model-based techniques, can ensure robustness and efficiency in pharmaceutical continuous manufacturing.

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