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基于低聚前体的温度诱导单分散、共价交联且可降解的聚(N-异丙基丙烯酰胺)微凝胶的组装

Temperature-Induced Assembly of Monodisperse, Covalently Cross-Linked, and Degradable Poly(N-isopropylacrylamide) Microgels Based on Oligomeric Precursors.

作者信息

Sivakumaran Daryl, Mueller Eva, Hoare Todd

机构信息

Department of Chemical Engineering, McMaster University, 1280 Main St. W, Hamilton, Ontario, Canada L8S 4L7.

出版信息

Langmuir. 2015 Jun 2;31(21):5767-78. doi: 10.1021/acs.langmuir.5b01421. Epub 2015 May 21.

Abstract

A simple, rapid, solvent-free, and scalable thermally driven self-assembly approach is described to produce monodisperse, covalently cross-linked, and degradable poly(N-isopropylacrylamide) (PNIPAM) microgels based on mixing hydrazide (PNIPAM-Hzd) and aldehyde (PNIPAM-Ald) functionalized PNIPAM precursors. Preheating of a seed PNIPAM-Hzd solution above its phase transition temperature produces nanoaggregates that are subsequently stabilized and cross-linked by the addition of PNIPAM-Ald. The ratio of PNIPAM-Hzd:PNIPAM-Ald used to prepare the microgels, the time between PNIPAM-Ald addition and cooling, the temperature to which the PNIPAM-Hzd polymer solution is preheated, and the concentration of PNIPAM-Hzd in the initial seed solution can all be used to control the size of the resulting microgels. The microgels exhibit similar thermal phase transition behavior to conventional precipitation-based microgels but are fully degradable into oligomeric precursor polymers. The microgels can also be lyophilized and redispersed without any change in colloidal stability or particle size and exhibit no significant cytotoxicity in vitro. We anticipate that microgels fabricated using this approach may facilitate translation of the attractive properties of such microgels in vivo without the concerns regarding microgel clearance that exist with other PNIPAM-based microgels.

摘要

本文描述了一种简单、快速、无溶剂且可扩展的热驱动自组装方法,用于制备基于酰肼(PNIPAM-Hzd)和醛(PNIPAM-Ald)功能化的PNIPAM前体混合的单分散、共价交联且可降解的聚(N-异丙基丙烯酰胺)(PNIPAM)微凝胶。将种子PNIPAM-Hzd溶液预热至其相变温度以上会产生纳米聚集体,随后通过添加PNIPAM-Ald使其稳定并交联。用于制备微凝胶的PNIPAM-Hzd与PNIPAM-Ald的比例、添加PNIPAM-Ald后至冷却的时间、PNIPAM-Hzd聚合物溶液预热的温度以及初始种子溶液中PNIPAM-Hzd的浓度,均可用于控制所得微凝胶的尺寸。这些微凝胶表现出与传统沉淀法微凝胶相似的热相变行为,但可完全降解为低聚前体聚合物。这些微凝胶还可以冻干并重新分散,而不会改变其胶体稳定性或粒径,并且在体外没有明显的细胞毒性。我们预计,使用这种方法制备的微凝胶可能有助于将此类微凝胶的诱人特性转化到体内,而无需担心其他基于PNIPAM的微凝胶存在的微凝胶清除问题。

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