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采用喷雾干燥技术制备的含有醋酸奥曲肽的颗粒状碎片,用于干粉吸入。

Fragmented particles containing octreotide acetate prepared by spray drying technique for dry powder inhalation.

机构信息

School of Pharmaceutical Sciences, Sun Yat-sen University, 132 East Circle at University Town, Guangzhou, 510006, China.

Institute for Biomedical and Pharmaceutical Sciences, Guangdong University of Technology, Guangzhou, China.

出版信息

Drug Deliv Transl Res. 2018 Jun;8(3):693-701. doi: 10.1007/s13346-018-0515-7.

Abstract

Dry powder inhalers (DPIs) have been proposed as an alternative administration route for protein and peptide drugs. However, DPI particles are easy to aggregate due to the strong interactions between the particles, leading to poor aerosolization performance. In this study, fragmented particles containing octreotide acetate (OA) were prepared by spray drying technique for dry powder inhalation, which were expected to decrease the particle-particle interaction by reducing the contact sites. Mannitol and ammonium carbonate were used as protein stabilizer and fragment-forming agent, respectively. The obtained fragmented particles presented larger particle size, lower density, better dispersibility, and well in vitro aerodynamic behavior (emitted dose > 97%, fine particle fraction ≈ 40%). The circular dichroism spectrum results indicated that OA maintained the stability throughout the spray drying process. The relative bioavailability of dry powder inhalation (DPI) compared with subcutaneous injection of commercial product was up to 88.0%, demonstrating the feasibility of DPI for OA delivery. These results confirmed that the proposed fragmented particles had great potential for pulmonary delivery of protein and peptide drugs in a painless, rapid, and convenient manner.

摘要

干粉吸入器(DPIs)已被提议作为蛋白质和肽类药物的替代给药途径。然而,由于颗粒之间的强相互作用,DPI 颗粒很容易聚集,导致气溶胶化性能不佳。在这项研究中,通过喷雾干燥技术制备了含有醋酸奥曲肽(OA)的碎粒,预计通过减少接触点来降低颗粒间的相互作用。甘露醇和碳酸铵分别用作蛋白质稳定剂和成粒剂。所得到的碎粒表现出更大的粒径、更低的密度、更好的分散性和良好的体外空气动力学行为(发射剂量>97%,细颗粒分数≈40%)。圆二色光谱结果表明,OA 在整个喷雾干燥过程中保持稳定。干粉吸入(DPI)与商业产品皮下注射的相对生物利用度高达 88.0%,表明 DPI 用于 OA 传递的可行性。这些结果证实,所提出的碎粒具有以无痛、快速和方便的方式将蛋白质和肽类药物递送至肺部的巨大潜力。

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