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Amorphous Calcium Carbonate Based-Microparticles for Peptide Pulmonary Delivery

机译:非晶态碳酸钙基微粒对肺部肽的输送

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Amorphous calcium carbonate (ACC) is known to interact with proteins, for example, in biogenic ACC, to form stable amorphous phases. The control of amorphous/crystalline and inorganic/organic ratios in inhalable calcium carbonate microparticles may enable particle properties to be adapted to suit the requirements of dry powders for pulmonary delivery by oral inhalation. For example, an amorphous phase can immobilize and stabilize polypeptides in their native structure and amorphous and crystalline phases have different mechanical properties. Therefore, inhalable composite microparticles made of inorganic (i.e., calcium carbonate and calcium formate) and organic (i.e., hyaluronan (HA)) amorphous and crystalline phases were investigated for peptide and protein pulmonary aerosol delivery. The crystalline/amorphous ratio and polymorphic form of the inorganic component was altered by changing the microparticle drying rate and by changing the ammonium carbonate and HA initial concentration. The bioactivity of the model peptide, salmon calcitonin (sCT), coprocessed with alpha-1-antitrypsin (AAT), a model protein with peptidase inhibitor activity, was maintained during processing and the microparticles had excellent aerodynamic properties, making them suitable for pulmonary aerosol delivery. The bioavailability of sCT after aerosol delivery as sCT and AAT-loaded composite microparticles to rats was 4-times higher than that of sCT solution.
机译:已知无定形碳酸钙(ACC)与蛋白质相互作用,例如在生物成因的ACC中,形成稳定的无定形相。可吸入碳酸钙微粒中无定形/结晶和无机/有机比例的控制可以使颗粒性质适应于通过口服吸入用于肺部递送的干粉的要求。例如,无定形相可以以其天然结构固定和稳定多肽,而无定形和结晶相具有不同的机械性能。因此,研究了由无机(即,碳酸钙和甲酸钙)和有机(即,透明质酸(HA))无定形和结晶相组成的可吸入复合微粒用于肽和蛋白质肺气雾剂的递送。通过改变微粒的干燥速率,改变碳酸铵和HA的初始浓度,可以改变无机组分的结晶/非晶比和多晶形式。模型肽鲑鱼降钙素(sCT)与具有肽酶抑制剂活性的模型蛋白alpha-1-antitrypsin(AAT)共同​​加工的生物活性在加工过程中得以保持,并且微粒具有出色的空气动力学特性,使其适合于肺气雾剂交货。气溶胶输送后,sCT的生物利用度是sCT和载有AAT的复合微粒对大鼠的生物利用度,是sCT溶液的4倍。

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