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Nanofiltration-based diafiltration process for solvent exchange in pharmaceutical manufacturing

机译:基于纳滤的渗滤工艺,用于制药生产中的溶剂交换

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Athermal solvent exchange from one organic synthesis step to the next step is highly desirable in bulk pharmaceutical manufacturing due to the thermally labile nature of the active intermediates. Diafiltration (DF) was employed using methanol as the solvent needed in the next synthesis step to drastically reduce the concentration of ethyl acetate used as the solvent in the previous synthesis step. Ethyl acetate was reduced to the level of a low concentration impurity in methanol by both batch and continuous DF using solvent resistant nanofiltration membranes MPF-50 and MPF-60; the latter has a high rejection of around 96% for the solute, erythromycin, representing an active intermediate. Nanofiltration-based diafiltration for exchanging the solvent methanol for ethyl acetate was demonstrated. The membrane rejection of the solute needs to be higher. Membrane compaction has to be considered in the design of the process for both membranes.
机译:由于活性中间体的热不稳定特性,在批量药物生产中非常需要从一个有机合成步骤到下一步骤的热溶剂交换。使用甲醇作为下一个合成步骤所需的溶剂进行渗滤(DF),以大大降低在上一个合成步骤中用作溶剂的乙酸乙酯的浓度。使用耐溶剂的纳滤膜MPF-50和MPF-60,通过分批和连续DF将乙酸乙酯的甲醇含量降低到低浓度杂质水平;后者对代表活性中间体的溶质红霉素有很高的排斥率,约为96%。证明了基于纳滤的渗滤,用于将溶剂甲醇交换为乙酸乙酯。溶质的膜截留率需要更高。在设计两种膜的过程中都必须考虑膜的压实。

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