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制备具有精确控制且单分散尺寸分布的聚乳酸-乙醇酸共聚物微球。

Fabrication of PLG microspheres with precisely controlled and monodisperse size distributions.

作者信息

Berkland C, Kim K, Pack D W

机构信息

Department of Chemical Engineering, University of Illinois, Urbana, IL 61801, USA.

出版信息

J Control Release. 2001 May 18;73(1):59-74. doi: 10.1016/s0168-3659(01)00289-9.

Abstract

The size distribution of biodegradable polymer microspheres critically impacts the allowable routes of administration, biodistribution, and release rate of encapsulated compounds. We have developed a method for producing microspheres of precisely controlled and/or monodisperse size distributions. Our apparatus comprises spraying a polymer-containing solution through a nozzle with (i) acoustic excitation to produce uniform droplets, and (ii) an annular, non-solvent carrier stream allowing further control of the droplet size. We used this apparatus to fabricate poly(D,L-lactide-co-glycolide) (PLG) spheres. The acoustic excitation method, by itself, produced uniform microspheres as small as 30 microm in diameter in which > or =95% of the spheres were within 1.0-1.5 microm of the average. The carrier stream method alone allowed production of spheres as small as approximately 1-2 microm in diameter from a 100-microm diameter nozzle, but generated broader size distributions. By combining the two devices, we fabricated very uniform spheres with average diameters from approximately 5 to >500 microm. Furthermore, by discretely or continuously varying the experimental parameters, we fabricated microsphere populations with predefined size distributions. Finally, we demonstrate encapsulation and in vitro release of a model drug compound, rhodamine B. In summary, our apparatus provides unprecedented control of microsphere size and may allow development of advanced controlled-release delivery systems.

摘要

可生物降解聚合物微球的尺寸分布对允许的给药途径、生物分布以及包封化合物的释放速率有着至关重要的影响。我们已经开发出一种用于生产尺寸分布精确可控和/或单分散的微球的方法。我们的装置包括通过一个喷嘴喷射含聚合物溶液,其中(i)采用声激发以产生均匀的液滴,以及(ii)采用环形非溶剂载流以进一步控制液滴尺寸。我们使用该装置制造聚(D,L-丙交酯-共-乙交酯)(PLG)微球。仅声激发方法就能产生直径小至30微米的均匀微球,其中≥95%的微球直径在平均直径的1.0 - 1.5微米范围内。仅载流方法能从100微米直径的喷嘴生产出直径小至约1 - 2微米的微球,但产生的尺寸分布更宽。通过将这两种装置结合,我们制造出了平均直径约为5至>500微米的非常均匀的微球。此外,通过离散或连续改变实验参数,我们制造出了具有预定义尺寸分布的微球群体。最后,我们展示了一种模型药物化合物罗丹明B的包封和体外释放。总之,我们的装置提供了对微球尺寸前所未有的控制,并且可能有助于开发先进的控释给药系统。

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