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刺激响应型抗氧化药物晶体及其生态意义。

Stimulus-Responsive Anti-Oxidizing Drug Crystals and their Ecological Implication.

机构信息

Department of Chemical and Biomolecular Engineering, University of Illinois at Urbana-Champaign, Illinois, 61801, United States.

Carl R. Woese Institute for Genomic Biology, Beckman Institute for Science and Technology, University of Illinois at Urbana-Champaign, Illinois, 61801, United States.

出版信息

Small. 2019 May;15(21):e1900765. doi: 10.1002/smll.201900765. Epub 2019 Apr 5.

Abstract

Various antioxidants are being used to neutralize the harmful effects of reactive oxygen species (ROS) overproduced in diseased tissues and contaminated environments. Polymer-directed crystallization of antioxidants has attracted attention as a way to control drug efficacy through molecular dissolution. However, most recrystallized antioxidants undertake continuous dissolution independent of the ROS level, thus causing side-effects. This study demonstrates a unique method to assemble antioxidant crystals that modulate their dissolution rate in response to the ROS level. We hypothesized that antioxidants recrystallized using a ROS-labile polymer would be triggered to dissolve when the ROS level increases. We examined this hypothesis by using catechin as a model antioxidant. Catechin was recrystallized using polyethylenimine cross-linked with ROS-labile diselanediylbis-(ethane-2,1-diyl)-diacrylate. Catechin crystallized with the ROS-labile polymer displays accelerated dissolution proportional to the H O concentration. The ROS-responsive catechin crystals protect vascular cells from oxidative insults by activating intracellular glutathione peroxidase expression and, in turn, inhibiting an increase in the intracellular oxidative stress. In addition, ROS-responsive catechin crystals alleviate changes in the heart rate of Daphnia magna in oxidative media. We propose that the results of this study would be broadly useful for improving the therapeutic efficacy of a broad array of drug compounds.

摘要

各种抗氧化剂被用于中和疾病组织和污染环境中过量产生的活性氧(ROS)的有害影响。抗氧化剂的聚合物导向结晶作为一种通过分子溶解控制药物功效的方法引起了人们的关注。然而,大多数重结晶的抗氧化剂独立于 ROS 水平进行持续溶解,从而导致副作用。本研究展示了一种独特的方法来组装抗氧化剂晶体,使其溶解速率能够响应 ROS 水平进行调节。我们假设使用 ROS 不稳定聚合物重结晶的抗氧化剂在 ROS 水平升高时会被触发溶解。我们使用儿茶素作为模型抗氧化剂来检验这一假设。儿茶素使用与 ROS 不稳定的二硒二基双(乙烷-2,1-二基)二丙烯酸酯交联的聚乙烯亚胺进行重结晶。与 ROS 不稳定聚合物结晶的儿茶素显示出与 H2O2浓度成正比的加速溶解。ROS 响应性儿茶素晶体通过激活细胞内谷胱甘肽过氧化物酶的表达来保护血管细胞免受氧化损伤,从而抑制细胞内氧化应激的增加。此外,ROS 响应性儿茶素晶体减轻了 Daphnia magna 在氧化介质中心率的变化。我们提出,这项研究的结果将广泛用于提高多种药物化合物的治疗效果。

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