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微流控辅助(PEG 化)聚(丙交酯-共-己内酯)的纳米沉淀:大分子和微流控参数对粒径和紫杉醇包封的影响。

Microfluidic-assisted nanoprecipitation of (PEGylated) poly (d,l-lactic acid-co-caprolactone): Effect of macromolecular and microfluidic parameters on particle size and paclitaxel encapsulation.

机构信息

North West Centre for Advanced Drug Delivery (NoWCADD), Division of Pharmacy & Optometry, School of Health Sciences, Medicine and Health, Stopford Building, Manchester M13 9PT, United Kingdom.

North West Centre for Advanced Drug Delivery (NoWCADD), Division of Pharmacy & Optometry, School of Health Sciences, Medicine and Health, Stopford Building, Manchester M13 9PT, United Kingdom.

出版信息

Int J Pharm. 2018 Sep 5;548(1):530-539. doi: 10.1016/j.ijpharm.2018.07.031. Epub 2018 Jul 17.

Abstract

In this work we evaluate the effect of polymer composition and architecture of (PEGylated) polyesters on particle size and paclitaxel (PTX) loading for particles manufactured via microfluidic-assisted, continuous-flow nanoprecipitation using two microfluidic chips with different geometries and mixing principles. We have prepared poly (d,l-lactic acid-co-caprolactone) (PLCL) from ring-opening polymerization (ROP) of LA and CL mixtures and different (macro) initiators (namely, 1-dodecanol, a MeO-PEG-OH, and a 4-armed star PEG-OH), rendering polyesters that vary in monomer composition (i.e. LA/CL ratios) and architecture (i.e. linear vs 4-armed star). Continuous-flow nanoprecipitation was assayed using two microfluidic chips: a cross-flow chip with a X-shaped mixing junction (2D laminar flow focusing) and a micromixer featuring a Y-shaped mixing junction and a split and recombine path (2D laminar flow focusing convinced with stream lamination for faster mixing). Nanoparticle formulations were produced with Z-average sizes in the range of 30-160 nm, although size selectivity could be seen for different polymer/chip combinations; for instance, smaller particles were obtained with Y-shaped micromixer (30-120 nm), specially for the PEGylated polyesters (30-50 nm), whereas the cross-flow chip systematically produced larger particles (80-160 nm). Loading of the anti-cancer drug paclitaxel (PTX) was also heavily influenced not only by the nature of the polyester, but also by the geometry of the microfluidic chip; higher drug loadings were obtained with the cross-flow reactor and the star block copolymers. Finally, decreasing the LA/CL ratio generally had a positive effect on drug loading.

摘要

在这项工作中,我们评估了(PEG 化)聚酯的聚合物组成和结构对通过使用具有不同几何形状和混合原理的两个微流控芯片的微流控辅助连续流纳米沉淀制造的颗粒的粒径和紫杉醇(PTX)负载的影响。我们已经通过开环聚合(ROP)由 LA 和 CL 混合物和不同的(大)引发剂(即 1-十二醇,MeO-PEG-OH 和 4 臂星 PEG-OH)制备了聚(DL-丙交酯-共-己内酯)(PLCL),得到了在单体组成(即 LA/CL 比)和结构(即线性与 4 臂星)上有所不同的聚酯。使用两个微流控芯片进行连续流纳米沉淀:具有 X 形混合接头(二维层流聚焦)的十字流芯片和具有 Y 形混合接头以及分裂和重组路径的微混合器(二维层流聚焦与流层化结合以实现更快的混合)。纳米颗粒制剂的 Z 均粒径在 30-160nm 范围内,尽管不同的聚合物/芯片组合可以看到粒径选择性;例如,Y 形微混合器(30-120nm)获得了较小的颗粒,特别是对于 PEG 化聚酯(30-50nm),而十字流芯片系统地产生了较大的颗粒(80-160nm)。抗癌药物紫杉醇(PTX)的负载也不仅受到聚酯性质的影响,还受到微流控芯片几何形状的影响;在十字流反应器和星形嵌段共聚物中获得了更高的药物负载。最后,降低 LA/CL 比通常对药物负载有积极影响。

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