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Technoeconomic optimisation and comparative environmental impact evaluation of continuous crystallisation and antisolvent selection for artemisinin recovery

机译:青蒿素回收的连续结晶和反溶剂选择的技术经济优化和比较环境影响评估

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Systematic nonlinear optimisation is a valuable tool towards evaluating the performance of conceptual Continuous Pharmaceutical Manufacturing (CPM) flowsheets. This study considers total cost minimisation of multiple plausible design choices and eight candidate antisolvents for the continuous recovery of artemisinin (a potent antimalarial Active Pharmaceutical Ingredient/API) via continuous crystallisation, with simultaneous evaluation of process mass and environmental efficiency via the E-factor (an established green chemistry metric). Essential design variables include the crystallisation cooling temperature, the antisolvent requirements and the use of multiple crystallisers in series. Acetonitrile achieves the minimum total cost for one crystalliser (761 • 10~3 GBP, for a crystallisation at 5 ℃, with 80% antisolvent addition and an E-factor of 29.1). The use of a second crystalliser in series allows for further total cost savings for all antisolvents; E-factors continue to decrease accordingly, albeit with very limited scope for each successive crystalliser due to negligible productivity improvements.
机译:系统的非线性优化是评估概念性连续药物制造(CPM)流程图性能的宝贵工具。这项研究考虑了通过多种可行的设计选择和八种候选抗溶剂的总成本最小化,以通过连续结晶连续回收青蒿素(一种有效的抗疟疾活性药物成分/ API),同时通过E因子同时评估工艺质量和环境效率(已建立的绿色化学指标)。基本的设计变量包括结晶冷却温度,抗溶剂要求以及串联使用多个结晶器。乙腈达到了一个结晶器的最低总成本(761•10〜3 GBP,在5℃结晶,加入80%的抗溶剂和29.1的E系数)。串联使用第二个结晶器可以进一步节省所有抗溶剂的总成本;尽管由于生产率的提高可忽略不计,但每个连续结晶器的作用范围非常有限,因此电子因子仍在继续降低。

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