The development and validation of a quality by design based process analytical tool for the inline quantification of Ramipril during hot-melt extrusion

Suha M Dadou; Zoe Senta-Loys; Ammar Almajaan; Shu Li; David S Jones; Anne M Healy; Yiwei Tian; Gavin P Andrews

doi:10.1016/j.ijpharm.2020.119382

The development and validation of a quality by design based process analytical tool for the inline quantification of Ramipril during hot-melt extrusion

Int J Pharm. 2020 Jun 30:584:119382. doi: 10.1016/j.ijpharm.2020.119382. Epub 2020 Apr 28.

Authors

Suha M Dadou¹, Zoe Senta-Loys¹, Ammar Almajaan¹, Shu Li¹, David S Jones¹, Anne M Healy², Yiwei Tian¹, Gavin P Andrews³

Affiliations

¹ Pharmaceutical Engineering Group, School of Pharmacy, Queen's University Belfast, Belfast, United Kingdom.
² School of Pharmacy and Pharmaceutical Sciences, Trinity College Dublin, Dublin, Ireland.
³ Pharmaceutical Engineering Group, School of Pharmacy, Queen's University Belfast, Belfast, United Kingdom. Electronic address: g.andrews@qub.ac.uk.

PMID: 32360547
DOI: 10.1016/j.ijpharm.2020.119382

Abstract

Continuous processing is superseding conventional batch processing as a means of manufacturing within the pharmaceutical research/industry. This paradigm shift has led to the implementation of Process Analytical Technology (PAT) as a semi-automatic, predictive tool offering real-time quality control that can be built into the production line. However, PAT tools have been mainly utilised to monitor a single process (e.g. powder blending, synthesis of biopharmaceuticals and small molecules) rather than a full continuous manufacturing process. In addition, there is a paucity of guidance documents that consider the continuous and dynamic conditions of real-time measurements for validation purposes. In this study, the feasibility of developing and validating a predictive and reliable Raman method based on quality by design (QbD) and PAT frameworks for the real-time quantification of Ramipril (RMP) during hot-melt extrusion (HME) were investigated. Through QbD, a design space elucidating the quality attributes of RMP stability was successfully identified based on offline HPLC measurements. Process temperature and powder feeding rate were the main quality attributes to affect the stability of RMP during HME. The optimum combination of process and formulation variables were extracted from the validated design space and used to extrude RMP at a concentration range of 2.5-12.5 %w/w. Three calibration models were established using PLS regression analysis. The developed PLS calibration models showed excellent linearity (R2 = 0.989, 0.995, 0.992), accuracy (RMSEcv = 0.31, 0.26, 0.30%) and specificity (PC1 = 81, 85, 89%) for models 1, 2 and 3, respectively. Furthermore, the developed QbD-PAT model was able to predict the quantity of RMP at varied process feed rate (10, 35 rpm) operating under long processing time (60 min). The output of this study allows in-process optimisation of formulation and process variables to control the quality and quantity of RMP during HME. Furthermore, it allows the implementation of PAT tools as routine methods of analysis within the laboratory.

Keywords: Chemometrics; Continuous manufacturing; Hot melt extrusion; Inline Raman spectroscopy; Process analytical technology; Quality by design.

MeSH terms

Dose-Response Relationship, Drug
Hot Temperature
Polymethacrylic Acids / chemistry*
Principal Component Analysis
Quality Control
Ramipril / administration & dosage*
Ramipril / chemistry
Spectroscopy, Near-Infrared
Spectrum Analysis, Raman
Technology, Pharmaceutical / methods*
Technology, Pharmaceutical / standards

Substances

Polymethacrylic Acids
methylmethacrylate-methacrylic acid copolymer
Ramipril