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Triggered Release of Loads from Microcapsule-in-Microcapsule Hydrogel Microcarriers: En-Route to an 'Artificial Pancreas'

机译:从微胶囊中的微胶囊水凝胶微载体触发释放的负荷:途中'人造胰腺'。

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摘要

A method to assemble stimuli-responsive nucleic acid-based hydrogel-stabilized micro-capsule-in-microcapsule systems is introduced. An inner aqueous compartment stabilized by a stimuli-responsive hydrogel-layer (~150 nm) provides the inner microcapsule (diameter ~2.5 μm). The inner microcapsule is separated from an outer aqueous compartment stabilized by an outer stimuli-responsive hydrogel layer (thickness of ~150 nm) that yields the microcapsule-in-microcapsule system. Different loads, e.g., tetramethyl rhodamine-dextran (TMR-D) and CdSe/ZnS quantum dots (QDs), are loaded in the inner and outer aqueous compartments. The hydrogel layers exist in a higher stiffness state that prevents inter-reservoir or leakage of the loads from the respective aqueous compartments. Subjecting the inner hydrogel layer to Zn~(2+)-ions and/or the outer hydrogel layer to acidic pH or crown ether leads to the triggered separation of the bridging units associated with the respective hydrogel layers. This results in the hydrogel layers of lower stiffness allowing either the mixing of the loads occupying the two aqueous compartments, the guided release of the load from the outer aqueous compartment, or the release of the loads from the two aqueous compartments. In addition, a pH-responsive microcapsule-in-microcapsule system is loaded with glucose oxidase (GOx) in the inner aqueous compartment and insulin in the outer aqueous compartment. Glucose permeates across the two hydrogel layers resulting in the GOx catalyzed aerobic oxidation of glucose to gluconic acid. The acidification of the microcapsule-in-microcapsule system leads to the triggered unlocking of the outer, pH-responsive hydrogel layer and to the release of insulin. The pH-stimulated release of insulin is controlled by the concentration of glucose. While at normal glucose levels, the release of insulin is practically prohibited, the dose-controlled release of insulin in the entire diabetic range is demonstrated. Also, switchable ON/OFF release of insulin is achieved highlighting an autonomous glucose-responsive microdevice operating as an "artificial pancreas" for the release of insulin.
机译:介绍了一种组装基于刺激响应核酸的水凝胶稳定的微胶囊中微胶囊系统的方法。由刺激响应水凝胶层(约150 nm)稳定的内部水室提供了内部微囊(直径约2.5μm)。内部微胶囊与外部水相隔间隔开,外部水相隔间由外部刺激响应水凝胶层(厚度约为150 nm)稳定,产生了微胶囊-微胶囊系统。在内部和外部水室中加载不同的负载,例如四甲基若丹明-葡聚糖(TMR-D)和CdSe / ZnS量子点(QDs)。水凝胶层以较高的刚性状态存在,这防止了储层之间或负载从各个含水隔室泄漏。使内部水凝胶层经​​受Zn〜(2 +)-离子和/或使外部水凝胶层经​​受酸性pH或冠醚,导致触发了与各个水凝胶层相关的桥连单元的分离。这导致水凝胶层具有较低的刚度,从而允许占据两个水性隔室的负载混合,从外部水性隔室的负载的引导释放或从两个水性隔室的负载的释放。此外,pH响应型微胶囊中微胶囊系统在内部水室中装有葡萄糖氧化酶(GOx),在外部水室中装有胰岛素。葡萄糖渗透穿过两个水凝胶层,导致GOx催化将葡萄糖有氧氧化为葡萄糖酸。微囊中微囊系统的酸化导致外部的,对pH敏感的水凝胶层的触发解锁以及胰岛素的释放。 pH刺激的胰岛素释放受葡萄糖浓度控制。在正常葡萄糖水平下,实际上禁止胰岛素的释放,但已证明在整个糖尿病范围内胰岛素的剂量控制释放。而且,实现了胰岛素的可开关的ON / OFF释放,突出了自主葡萄糖响应微设备的功能,该微设备充当用于释放胰岛素的“人造胰腺”。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2020年第9期|4223-4234|共12页
  • 作者

  • 作者单位

    Institute of Chemistry Center for Nanoscience and Nanotechnology The Hebrew University of Jerusalem Jerusalem 91904 Israel;

    Institute of Life Science The Hebrew University of Jerusalem Jerusalem 91904 Israel;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
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  • 入库时间 2022-08-18 05:22:34

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