Linked experimental and modelling approaches for tablet property predictions

外推法 压实 组分(热力学) 设计质量 压缩(物理) 体积热力学 计算机科学 工艺工程 混合(物理) 二进制数 实验数据 生物系统 材料科学 数学 热力学 化学 统计 工程类 粒径 复合材料 物理 算术 物理化学 量子力学 生物
作者
Hikaru G. Jolliffe,Ebenezer Ojo,Carlota Mendez Torrecillas,Ian Houson,Richard Elkes,Gavin Reynolds,Angela Kong,E. J. Meehan,Felipe Amado Becker,Patrick M. Piccione,Sudhir Kumar Verma,Aditya Singaraju,Gavin Halbert,John Robertson
出处
期刊:International Journal of Pharmaceutics [Elsevier BV]
卷期号:626: 122116-122116 被引量:8
标识
DOI:10.1016/j.ijpharm.2022.122116
摘要

Recent years have seen the advent of Quality-by-Design (QbD) as a philosophy to ensure the quality, safety, and efficiency of pharmaceutical production. The key pharmaceutical processing methodology of Direct Compression to produce tablets is also the focus of some research. The traditional Design-of-Experiments and purely experimental approach to achieve such quality and process development goals can have significant time and resource requirements. The present work evaluates potential for using combined modelling and experimental approach, which may reduce this burden by predicting the properties of multicomponent tablets from pure component compression and compaction model parameters. Additionally, it evaluates the use of extrapolation from binary tablet data to determine theoretical pure component model parameters for materials that cannot be compacted in the pure form. It was found that extrapolation using binary tablet data - where one known component can be compacted in pure form and the other is a challenging material which cannot be - is possible. Various mixing rules have been evaluated to assess which are suitable for multicomponent tablet property prediction, and in the present work linear averaging using pre-compression volume fractions has been found to be the most suitable for compression model parameters, while for compaction it has been found that averaging using a power law equation form produced the best agreement with experimental data. Different approaches for estimating component volume fractions have also been evaluated, and using estimations based on theoretical relative rates of compression of the pure components has been found to perform slightly better than using constant volume fractions (that assume a fully compressed mixture). The approach presented in this work (extrapolation of, where necessary, binary tablet data combined with mixing rules using volume fractions) provides a framework and path for predictions for multicomponent tablets without the need for any additional fitting based on the multicomponent formulation composition. It allows the knowledge space of the tablet to be rapidly evaluated, and key regions of interest to be identified for follow-up, targeted experiments that that could lead to an establishment of a design and control space and forgo a laborious initial Design-of-Experiments.

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