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Use of Continuous MSMPR Crystallization with Integrated Nanofiltration Membrane Recycle for Enhanced Yield and Purity in API Crystallization

机译:连续MSMPR结晶与集成的纳滤膜再循环的结合使用,可提高API结晶的收率和纯度

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If continuous processing is to be employed in pharmaceutical production, it is essential that continuous crystallization techniques can meet the purity and yield achievable in current batch crystallization processes. Recycling of mother liquor in steady state MSMPR crystallizations allows the yield in the equivalent equilibrium batch process to be met or exceeded. However, the extent to which yield can be increased is limited by the buildup of impurities within the system. In this study, an organic solvent nanofiltration membrane was used to preferentially concentrate an API (deferasirox, M.W. = 373 Da) and purge the limiting impurity 4-hydrazinobenzoic acid (MW = 152 Da) from the mother liquor recycle stream in a mixed solvent (THF:ethanol) antisolvent (water) system. Incorporation of the membrane recycle allowed yields of 98.0% and 98.7% to be achieved. This compares to the following: a control MSMPR run without a membrane (70.3%), an equivalent batch process (89.2%), and the current commercial batch process (92%). Comparable product impurity levels were measured for the following: the MSMPR membrane recycle experiments (0.15 ppm and 0.22 ppm), the MSMPR control (0.13 ppm), and batch (0.32 ppm) control experiments. All processes met the regulatory specifications of a maximum of 3 ppm of the impurity 4-hydrainobenzoic acid.
机译:如果要在药品生产中采用连续加工,则连续结晶技术必须能够满足当前分批结晶过程中可获得的纯度和收率,这一点至关重要。稳定状态MSMPR结晶中的母液再循环,可以达到或超过等效平衡间歇法的收率。然而,产量增加的程度受到系统内杂质的积累的限制。在这项研究中,使用有机溶剂纳滤膜优先浓缩API(地拉罗司,MW = 373 Da),并在混合溶剂中从母液循环流中清除极限杂质4-肼基苯甲酸(MW = 152 Da)。 THF:乙醇)抗溶剂(水)体系。膜循环的并入使得可以达到98.0%和98.7%的产率。相比之下,没有膜的对照MSMPR(70.3%),等效的批处理(89.2%)和当前的商业批处理(92%)。测量了以下产品的可比较产品杂质水平:MSMPR膜循环实验(0.15 ppm和0.22 ppm),MSMPR对照(0.13 ppm)和批次(0.32 ppm)对照实验。所有过程均符合最大3 ppm的杂质4-氢苯甲酸的法规要求。

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