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水凝胶纳米颗粒网络的可控药物释放。

Controlled drug release from hydrogel nanoparticle networks.

作者信息

Huang Gang, Gao Jun, Hu Zhibing, St John John V, Ponder Bill C, Moro Dan

机构信息

Departments of Physics and Chemistry, University of North Texas, 211 Avenue A, Denton, TX 76203, USA.

出版信息

J Control Release. 2004 Feb 10;94(2-3):303-11. doi: 10.1016/j.jconrel.2003.10.007.

Abstract

Monodisperse nanoparticles of poly-N-isopropylacrylamide-co-allylamine (PNIPAM-co-allylamine) and PNIPAM-co-acrylic acid (PNIPAM-co-AA) were synthesized. The close-packed PNIPAM-co-allylamine and PNIPAM-co-AA nanoparticles were converted to three-dimensional gel networks by covalently crosslinking neighboring particles at room temperature and neutral pH using glutaric dialdehyde and adipic acid dihydrazide, respectively. Controlled release studies were conducted using dextran markers of various molecular weights as model macromolecular drugs. Release was quantified under various physical conditions, including a range of temperatures and dextran molecular weights. Dextran, entrapped in cavities in the nanoparticle network, was released with a rate regulated by their molecular weights and cavity size. No release from a conventional bulk PNIPAM gel, with high crosslinking density, was observed. The rate of release from the PNIPAM-co-allylamine network was temperature-dependent, being much faster at room temperature than that at human body temperature. In contrast, release of low molecular weight dextrans from the PNIPAM-co-AA network showed a temperature-independent release profile. These nanoparticle networks have several advantages over conventional bulk gels for controlling the release of high molecular weight biomolecules.

摘要

合成了聚-N-异丙基丙烯酰胺-共-烯丙胺(PNIPAM-共-烯丙胺)和聚-N-异丙基丙烯酰胺-共-丙烯酸(PNIPAM-共-AA)的单分散纳米颗粒。紧密堆积的PNIPAM-共-烯丙胺和PNIPAM-共-AA纳米颗粒分别在室温及中性pH条件下,使用戊二醛和己二酸二酰肼将相邻颗粒共价交联,从而转化为三维凝胶网络。使用各种分子量的葡聚糖标记物作为模型大分子药物进行控释研究。在包括一系列温度和葡聚糖分子量在内的各种物理条件下对释放进行定量。包裹在纳米颗粒网络腔中的葡聚糖以受其分子量和腔大小调节的速率释放。未观察到具有高交联密度的常规本体PNIPAM凝胶有释放现象。PNIPAM-共-烯丙胺网络的释放速率与温度有关,在室温下比在人体温度下快得多。相比之下,低分子量葡聚糖从PNIPAM-共-AA网络的释放显示出与温度无关的释放曲线。与传统本体凝胶相比,这些纳米颗粒网络在控制高分子量生物分子的释放方面具有几个优点。

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