Implementation of the Quality by Design approach for developing the composition and the manufacturing technology of an injectable drug for intra-articular introduction

News of Pharmacy Pub Date : 2021-02-01 DOI:10.24959/nphj.21.44

O. Saliy, O. Los, T. Palchevska, K. Nebylytsia

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Abstract

Aim. To implement the Quality by Design (QbD) approach in order to develop the composition and the manufacturing technology of injectable hyaluronate sodium (HS) in combination with chondroitin sulfate (CS) for intra-articularintroduction. Materials and methods. The composition of the solution for injection was developed using samples of the active pharmaceutical ingredient (API) of HS and CS. The approaches of the ICH international guidelines were used to create the QbD protocol. The quality target product profile (QTPP) was developed based on the literature review, analysis of similar drugs and the previous in-house experimental studies. Determination of critical quality assessment (CQA) product indicators was performed by risk analysis for all quality indicators listed in QTPP. The risk assessment of quality indicators was performed by assessing them according to the Risk Priority Number system (hereinafter – RPN) by a 9-point scale. When studying the composition and the manufacturing technology of the injectable solution the quality risk management (QRM) was developed according to the Ishikawa diagram. Results and discussion. It has been found that the QbD concept is a systematic approach to the drug development. At the first stage QTPP was developed. Based on the QTPP data the CQA indicators were determined, and quality risks were assessed. The critical process parameters (CPP) of the solution for injection based on HS and CS, their control methods, as well as the critical material attributes (CMA) were determined. Based on the data obtained the drug control strategy was proposed taking into account the need to minimize the repetition of control experiments. Using the Isikawa diagram the variability of the material and the process with the environmental factors affecting the qualityof the solution for injection with HS and CS was shown.Conclusions. Using the basic QbD approaches when developing the composition and the manufacturing technology of an injectable drug for intra-articular introduction it has been found that the route of administration, dose, potency, and consumer properties of the product are important aspects of QTPP. It has been proven that the quality indicators, such as transparency, viscosity, sterility and the quantitative content of API are determined as CQA to achieve the objectives defined in QTPP. The study shows that almost all stages of production are critical, therefore, they need to be constantly monitored and checked to obtain a quality product. In further experimental studies to confirm the composition developed and the manufacturing technology according to QRM it is necessary to focus on such indicators as the solution temperature, stabilization time, degassing mode and filtration conditions.

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用于开发关节内注射药物的组合物和制造技术的设计质量方法的实施

的目标。实施质量设计(QbD)方法，开发关节内注射用透明质酸钠(HS)联合硫酸软骨素(CS)的组成和生产工艺。材料和方法。使用HS和CS的活性药物成分(API)样品配制注射用溶液的组成。制定QbD方案时采用了ICH国际指南的方法。质量目标产品简介(QTPP)是在文献回顾、同类药物分析和之前的内部实验研究的基础上制定的。通过对QTPP中列出的所有质量指标进行风险分析，确定关键质量评价(CQA)产品指标。对质量指标进行风险评价，按照风险优先级编号系统(以下简称RPN)，采用9分制进行评价。在研究注射溶液的组成和制造工艺时，根据石川图建立了质量风险管理(QRM)。结果和讨论。研究发现，QbD概念是一种系统的药物开发方法。在第一阶段，QTPP得到了发展。根据QTPP数据确定了CQA指标，并对质量风险进行了评估。确定了基于HS和CS的注射液的关键工艺参数(CPP)及其控制方法，以及关键材料属性(CMA)。根据所获得的数据，提出了最小化控制实验重复的药物控制策略。用Isikawa图显示了影响HS和CS注射液质量的材料和工艺随环境因素的变异性。在开发关节内注射药物的组合物和制造技术时，使用基本的QbD方法已经发现，给药途径，剂量，效力和产品的消费者特性是QTPP的重要方面。实践证明，将原料药的透明度、粘度、无菌性、定量含量等质量指标确定为CQA，以达到QTPP中规定的目标。研究表明，几乎所有的生产阶段都是至关重要的，因此，他们需要不断地监控和检查，以获得高质量的产品。在进一步的实验研究中，根据QRM开发的成分和制造工艺，需要重点研究溶液温度、稳定时间、脱气方式和过滤条件等指标。

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News of Pharmacy

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