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酸改性复合氧载体CaSO_4-CaO的反应性能 被引量:4
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作者 钟思梅 郑敏 +1 位作者 邢艳彬 蒲思旭 《化工进展》 EI CAS CSCD 北大核心 2018年第4期1426-1432,共7页
将CaO添加到经不同酸改性后的CaSO_4氧载体中来制备CaSO_4-CaO复合氧载体。采用XRD、H_2-TPR、CO小型卧式管式炉开展恒温反应和循环实验,对氧载体进行表征和评价。主要研究了酸的种类对CO_2生成、气体硫化物的释放及复合氧载体循环反应... 将CaO添加到经不同酸改性后的CaSO_4氧载体中来制备CaSO_4-CaO复合氧载体。采用XRD、H_2-TPR、CO小型卧式管式炉开展恒温反应和循环实验,对氧载体进行表征和评价。主要研究了酸的种类对CO_2生成、气体硫化物的释放及复合氧载体循环反应性能的影响。结果表明:酸化的复合氧载体的氢气还原活性均明显优于未经改性过的CaSO_4,相比无酸化处理的CaSO_4氧载体,酸化后的CaSO_4-CaO复合氧载体,特别是HCl酸化,主要是提高了CaSO_4竞争还原副反应的选择性,导致主要气体硫化物SO_2释放显著增加,而COS释放略有降低。以CaCO_3煅烧得到的CaO与经HNO_3改性的CaSO_4进行机械混合制得的复合氧载体具有较好的反应活性,但是经过6次循环反应后,还原反应活性下降;循环反应中,气体硫化物主要来自于CaSO_4在还原阶段释放出的SO_2。 展开更多
关键词 复合氧载体 酸改性 CO2捕集 反应活性 SO2释放 cos释放
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Microencapsulation of immunoglobulin Y: optimization with response surface morphology and controlled release during simulated gastrointestinal digestion 被引量:3
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作者 Jin ZHANG Huan-huan LI +7 位作者 Yi-fan CHEN Li-hong CHEN Hong-gang TANG Fan-bin KONG Yun-xin YAO Xu-ming LIU Qian LAN Xiao-fan YU 《Journal of Zhejiang University-Science B(Biomedicine & Biotechnology)》 SCIE CAS CSCD 2020年第8期611-627,共17页
Immunoglobulin Y(Ig Y)is an effective orally administered antibody used to protect against various intestinal pathogens,but which cannot tolerate the acidic gastric environment.In this study,Ig Y was microencapsulated... Immunoglobulin Y(Ig Y)is an effective orally administered antibody used to protect against various intestinal pathogens,but which cannot tolerate the acidic gastric environment.In this study,Ig Y was microencapsulated by alginate(ALG)and coated with chitooligosaccharide(COS).A response surface methodology was used to optimize the formulation,and a simulated gastrointestinal(GI)digestion(SGID)system to evaluate the controlled release of microencapsulated Ig Y.The microcapsule formulation was optimized as an ALG concentration of 1.56%(15.6 g/L),COS level of 0.61%(6.1 g/L),and Ig Y/ALG ratio of 62.44%(mass ratio).The microcapsules prepared following this formulation had an encapsulation efficiency of 65.19%,a loading capacity of 33.75%,and an average particle size of 588.75μm.Under this optimum formulation,the coating of COS provided a less porous and more continuous microstructure by filling the cracks on the surface,and thus the GI release rate of encapsulated Ig Y was significantly reduced.The release of encapsulated Ig Y during simulated gastric and intestinal digestion well fitted the zero-order and first-order kinetics functions,respectively.The microcapsule also allowed the Ig Y to retain 84.37%immune-activity after 4 h simulated GI digestion,significantly higher than that for unprotected Ig Y(5.33%).This approach could provide an efficient way to preserve Ig Y and improve its performance in the GI tract. 展开更多
关键词 Immunoglobulin Y(IgY) MICROENCAPSULATION Chitooligosaccharide(cos) Response surface methodology(RSM) Controlled release Simulated gastrointestinal digestion(SGID)
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