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作 者:Mingxuan Li Suoqing Zhang Jiansong Wang Jiahui Li Wei Zhao Leida Zhang Mingyang Chen Dandan Han Junbo Gong
机构地区:[1]State Key Laboratory of Chemical Engineering,School of Chemical Engineering and Technology,Tianjin University,Tianjin,300072,China [2]Institute of Shaoxing,Tianjin University,Zhejiang,312300,China [3]Shandong Fuyang Biotechnology Co.,Ltd.,Shandong,253100,China [4]Haihe Laboratory of Sustainable Chemical Transformations,Tianjin,300192,China
出 处:《Particuology》2024年第11期158-172,共15页颗粒学报(英文版)
基 金:financially supported by the Key 647 Research and Development Project of Hebei 22372601D;the financial support of Haihe Laboratory of Sustainable Chemical Transformations.
摘 要:Regarding sugar and salt crystallization with large single crystals,the agglomerate thermodynamics and geometric morphologies,not the dynamics,dominate the particle size distribution(PSD).To consider this issue,a PSD design model is proposed for limited large crystal agglomeration.In this model,the agglomeration thermodynamic criticality is determined by estimating the adhesion and dispersion forces between single crystals.The geometric agglomerate morphologies are described by corresponding single crystal units stacking with porosity.By seed well-controlled of population,the key parameters of PSD(D01,D50 and D99)are precisely designed.For erythritol,the model design accuracies are 92%–99%in the 1.2 L and 10 L crystallizers,indicating that it can design PSD at various crystallization scales.Concerning the general research attention to microcrystal agglomeration kinetics(mostly active pharmaceutical ingredients),this model effectively guides the sugar and salt PSD design with limited large crystal agglomeration.
关 键 词:Particle size distribution design AGGLOMERATION Crystal geometric morphology Mathematic model ERYTHRITOL
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