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Preparation and in vivo absorption evaluation of spray dried powders containing salmon calcitonin loaded chitosan nanoparticles for pulmonary delivery

机译:载有降钙素的鲑鱼降钙素纳米颗粒的喷雾干燥粉末的制备及体内吸收评价

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Purpose: The aim of the present study was to prepare inhalable co-spray dried powders of salmon calcitonin loaded chitosan nanoparticles (sCT-CS-NPs) with mannitol and investigate pulmonary absorption in rats. Methods: The sCT-CS-NPs were prepared by the ionic gelation method using sodium tripolyphosphate (TPP) as a cross-linking polyion. Inhalable dry powders were obtained by co-spray drying aqueous dispersion of sCT-CS-NPs and mannitol. sCT-CS-NPs co-spray dried powders were characterized with respect to morphology, particle size, powder density, aerodynamic diameter, protein integrity, in vitro release of sCT, and aerosolization. The plasmatic sCT levels following intratracheal administration of sCT-CS-NPs spray dried powders to the rats was also determined. Results: sCT-CS-NPs were able to be incorporated into mannitol forming inhalable microparticles by the spray drying process. The sCT-CS-NPs/mannitol ratios and spray drying process affected the properties of the microparticles obtained. The conformation of the secondary structures of sCTs was affected by both mannitol content and spray dry inlet temperature. The sCT-CS-NPs were recovered after reconstitution of spray dried powders in an aqueous medium. The sCT release profile from spray dried powders was similar to that from sCT-CS-NPs. In vitro inhalation parameters measured by the Andersen cascade impactor indicated sCT-CS-NPs spray dried powders having promising aerodynamic properties for deposition in the deep lung. Determination of the plasmatic sCT levels following intratracheal administration to rats revealed that the inhalable sCT-CS NPs spray dried powders provided higher protein absorption compared to native sCT powders. Conclusion: The sCT-CS-NPs with mannitol based spray dried powders were prepared to have appropriate aerodynamic properties for pulmonary delivery. The developed system was able to deliver sCT via a pulmonary route into the systemic circulation.
机译:目的:本研究的目的是制备鲑鱼降钙素壳聚糖纳米粒(sCT-CS-NPs)与甘露醇的可喷雾共喷雾干燥粉末,并研究大鼠的肺吸收。方法:以三聚磷酸钠(TPP)为交联聚离子,通过离子凝胶法制备sCT-CS-NPs。通过共同喷雾干燥sCT-CS-NPs和甘露醇的水分散液获得可吸入的干粉。 sCT-CS-NPs共喷雾干燥粉末的形态,粒径,粉末密度,空气动力学直径,蛋白质完整性,sCT的体外释放和雾化特性得到了表征。还确定了向大鼠气管内施用sCT-CS-NPs喷雾干燥粉末后的血浆sCT水平。结果:sCT-CS-NPs可以通过喷雾干燥过程掺入形成甘露醇的可吸入微粒中。 sCT-CS-NPs /甘露醇的比例和喷雾干燥过程影响了所得微粒的性质。 sCTs二级结构的构象受甘露醇含量和喷雾干燥入口温度的影响。在水性介质中将喷雾干燥的粉末重构后,回收了sCT-CS-NP。喷雾干燥粉末的sCT释放曲线与sCT-CS-NPs相似。由Andersen级联撞击器测量的体外吸入参数表明,sCT-CS-NPs喷雾干燥的粉末具有良好的空气动力学特性,可沉积在深肺中。气管内给药大鼠后血浆sCT水平的测定表明,与天然sCT粉末相比,可吸入的sCT-CS NPs喷雾干燥粉末可提供更高的蛋白质吸收。结论:以甘露醇为基的喷雾干燥粉末制备的sCT-CS-NPs具有合适的空气动力学特性,可用于肺部递送。开发的系统能够通过肺部途径将sCT传递到全身循环中。

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