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Thermoresponsive hydrogels in biomedical applications.生物医学应用中的热响应水凝胶。
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Thermo- and pH-responsive polymers in drug delivery.药物递送中的热响应和pH响应聚合物。
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pH-sensitive hydrogels based on bovine serum albumin for oral drug delivery.基于牛血清白蛋白的pH敏感水凝胶用于口服药物递送。
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基于水解明胶的热敏性微球作为药物递送装置。

Negative thermo-responsive microspheres based on hydrolyzed gelatin as drug delivery device.

机构信息

Pharmaceutical Science Department, University of Calabria, Edificio Polifunzionale, Rende, (CS), Italy.

出版信息

AAPS PharmSciTech. 2010 Jun;11(2):652-62. doi: 10.1208/s12249-010-9429-5. Epub 2010 Apr 20.

DOI:10.1208/s12249-010-9429-5
PMID:20405255
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2902322/
Abstract

This paper deals with the synthesis of thermo-responsive microspheres with proteic structure exhibiting a transition temperature close to the body temperature. Temperature-sensitive hydrogels have attracted extensive interest due to their potential and promising applications in drug delivery field since they can undergo a rapid and reversible phase transition from a swollen to a shrunken state depending on environmental temperature. The hydrogels were synthesized by free-radical polymerization of hydrolyzed methacrylated gelatin (HGel-MA) and N,N'-methylenebisacrylamide as pro-hydrophilic multifunctional macromer and crosslinker, respectively, and N-isopropylacrylamide as thermo-responsive monomer. Thermal analyses showed negative thermo-responsive behavior for all compositions and, by increasing the content of the hydrophilic moieties in the network, the transition temperature raised to 36.9 degrees C, close to the physiological values. In order to test the materials as drug carriers, diclofenac sodium salt was chosen as model drug. Drug release profiles, in phosphate buffer solution (pH 7.0, 10(-3) M) at 25 and 40 degrees C, depend on the hydrogel's crosslinking degree and hydrophilic/hydrophobic balance in the polymeric network. For all formulations, in the shrunken state, the drug release percent values ranged from 80% to 100% after 24 h, and after 3 h, more than 60% of therapeutics was delivered. On the contrary, the swelling of the loaded microparticles produces, even after 30 h, a drug release percent of about 75%. By using semi-empirical equations, the release mechanism was extensively studied and the diffusional contribute was evaluated. The physico-chemical characteristics of thermo-responsive materials confirm the applicability of the microspheres as drug delivery device.

摘要

本文致力于合成具有蛋白质结构的温敏微球,这种微球具有接近体温的转变温度。温敏水凝胶由于其在药物输送领域的潜在和有前途的应用而引起了广泛的关注,因为它们可以根据环境温度从溶胀状态快速和可逆地转变为收缩状态。水凝胶是通过水解甲基丙烯酰化明胶(HGel-MA)和 N,N'-亚甲基双丙烯酰胺分别作为亲水性多功能大分子单体和交联剂,以及 N-异丙基丙烯酰胺作为温敏单体的自由基聚合合成的。热分析表明所有组成物均表现出负温敏行为,并且通过增加网络中亲水性部分的含量,转变温度升高至 36.9 摄氏度,接近生理值。为了测试材料作为药物载体的性能,选择双氯芬酸钠盐作为模型药物。在磷酸盐缓冲溶液(pH 7.0,10^-3 M)中,在 25 和 40 摄氏度下的药物释放曲线取决于水凝胶的交联度和聚合物网络中的亲水/疏水平衡。对于所有配方,在收缩状态下,在 24 小时后,药物释放百分比值在 80%到 100%之间,并且在 3 小时后,超过 60%的治疗剂被递送。相反,负载微球的溶胀产生了即使在 30 小时后,药物释放百分比仍约为 75%。通过使用半经验方程,广泛研究了释放机制并评估了扩散贡献。温敏材料的物理化学特性证实了微球作为药物输送装置的适用性。