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Optimization of batch antisolvent crystallization.

机译:批式反溶剂结晶的优化。

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Batch antisolvent crystallization is a commonly used crystallization method in the pharmaceutical industry, which produces very pure crystals with a narrow particle size distribution and high yields. It is also an effective method to crystallize heat sensitive materials, since the crystallization can be achieved at low temperatures.; The objectives of this research were to study the effect of the antisolvent addition rate on various crystallization parameters, including operational parameters and product specification parameters, and to find an operating procedure that produces a desired particle size distribution. The monitoring of the system is done in situ using attenuated total reflection Fourier transform infrared (ATR FTIR) spectroscopy.; Since antisolvent crystallisation involves two solvents, the polarity behavior of binary systems is addressed first. This involved the introduction of a spectroscopic method to estimate polarities of pure solvents. The same method was applied to binary mixtures. It was shown that even small amounts of antisolvent will cause significant nonideality in the polarity of the system. This should be accounted for in antisolvent crystallization.; The chosen crystallization was I-lysine monohydrochloride purification using water as a solvent and ethanol as an antisolvent. The solubility data for I-lysine monohydrochloride in water, ethanol, and mixtures of water and ethanol were determined. The addition of ethanol decreased the solubility of I-lysine monohydrochloride in water significantly.; The growth kinetics of I-lysine monohydrochloride were estimated from nucleation cell and seeded laboratory scale experiments. These data were used to predict nucleation rates. It was shown that the nucleation rate is very high throughout the crystallization.; The effect of the antisolvent addition rate on bulk supersaturation and particle size was studied. ATR FTIR spectroscopy was used to study the bulk supersaturation. It was shown that the bulk supersaturation was not a function of antisolvent concentration. Sieving showed that the particle size was strongly dependent on the antisolvent addition rate.; This dissertation employed a spectroscopic method for studying solvent polarity behavior. The feasibility of ATR FTIR spectroscopy for monitoring batch antisolvent crystallization was demonstrated. Also, an operating scheme for producing the desired particle size was presented.
机译:间歇式反溶剂结晶是制药工业中常用的结晶方法,可生产出粒径分布窄,产率高的非常纯净的晶体。这也是使热敏材料结晶的有效方法,因为可以在低温下实现结晶。这项研究的目的是研究抗溶剂添加量对各种结晶参数(包括操作参数和产品规格参数)的影响,并找到产生所需粒度分布的操作程序。使用衰减全反射傅立叶变换红外(ATR FTIR)光谱原位完成系统的监视。由于抗溶剂结晶涉及两种溶剂,因此首先要解决二元体系的极性行为。这涉及引入光谱法来估计纯溶剂的极性。将相同的方法应用于二元混合物。结果表明,即使少量的反溶剂也会在系统的极性上引起明显的非理想性。这应该在抗溶剂结晶中解决。选择的结晶是使用水作为溶剂,乙醇作为抗溶剂的1-赖氨酸一盐酸盐纯化。确定了赖氨酸一盐酸盐在水,乙醇以及水和乙醇的混合物中的溶解度数据。乙醇的加入显着降低了赖氨酸一盐酸盐在水中的溶解度。从成核细胞和种子实验室规模的实验中估算了I-赖氨酸盐酸盐的生长动力学。这些数据用于预测成核速率。结果表明,在整个结晶过程中,成核速率非常高。研究了抗溶剂添加速率对本体过饱和度和粒径的影响。 ATR FTIR光谱用于研究整体过饱和。结果表明,本体过饱和不是抗溶剂浓度的函数。筛分表明颗粒大小强烈取决于抗溶剂的添加速率。本文采用光谱方法研究了溶剂的极性行为。证明了ATR FTIR光谱法监测间歇式反溶剂结晶的可行性。此外,提出了产生所需粒度的操作方案。

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