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High throughput screening of particle conditioning operations: II. Evaluation of scale-up heuristics with prokaryotically expressed polysaccharide vaccines

机译:高通量筛选颗粒调节操作:II。用原核表达的多糖疫苗评估放大试探法

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Multivalent polysaccharide conjugate vaccines are typically comprised of several different polysaccharides produced with distinct and complex production processes. Particle conditioning steps, such as precipitation and flocculation, may be used to aid the recovery and purification of such microbial vaccine products. An ultra scale-down approach to purify vaccine polysaccharides at the micro-scale would greatly enhance productivity, robustness, and speed the development of novel conjugate vaccines. In part one of this series, we described a modular and high throughput approach to develop particle conditioning processes (HTPC) for biologicals that combines flocculation, solids removal, and streamlined analytics. In this second part of the series, we applied HTPC to industrially relevant feedstreams comprised of capsular polysaccharides (CPS) from several bacterial species. The scalability of HTPC was evaluated between 0.8mL and 13L scales, with several different scaling methodologies examined. Clarification, polysaccharide yield, impurity clearance, and product quality achieved with HTPC were reproducible and comparable with larger scales. Particle sizing was the response with greatest sensitivity to differences in processing scale and enabled the identification of useful scaling rules. Scaling with constant impeller tip speed or power per volume in the impeller swept zone offered the most accurate scale up, with evidence that time integration of these values provided the optimal basis for scaling. The capability to develop a process at the micro-scale combined with evidence-based scaling metrics provide a significant advance for purification process development of vaccine processes. The USD system offers similar opportunities for HTPC of proteins and other complex biological molecules. Biotechnol. Bioeng. 2015;112: 1568-1582. (c) 2015 Wiley Periodicals, Inc.
机译:多价多糖缀合物疫苗通常由几种不同的多糖组成,这些多糖以不同且复杂的生产过程生产。诸如沉淀和絮凝之类的颗粒调节步骤可用于帮助这种微生物疫苗产品的回收和纯化。在微型规模上纯化疫苗多糖的超规模缩减方法将大大提高生产率,稳健性,并加快新型结合疫苗的开发。在本系列的第1部分中,我们描述了一种模块化的高通量方法,用于开发结合了絮凝,去除固体和简化分析的生物制剂颗粒调节过程(HTPC)。在该系列的第二部分中,我们将HTPC应用于工业相关的饲料流中,该饲料流包含来自几种细菌物种的荚膜多糖(CPS)。 HTPC的可扩展性在0.8mL至13L的刻度范围内进行了评估,并考察了几种不同的缩放方法。 HTPC的澄清度,多糖收率,杂质清除率和产品质量均具有可重现性,可与更大规模的产品相媲美。粒度确定是对处理规模差异最敏感的响应,并能够确定有用的缩放规则。以恒定的叶轮尖端速度或叶轮后掠区域中的每体积功率进行缩放可提供最准确的缩放比例,并有证据表明这些值的时间积分为缩放提供了最佳基础。在微观规模上开发流程的能力与基于证据的缩放指标相结合,为疫苗流程的纯化流程开发提供了重大进展。美元系统为蛋白质和其他复杂生物分子的HTPC提供了类似的机会。生物技术。生恩2015; 112:1568-1582。 (c)2015年威利期刊有限公司

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