石墨烯结合透明质酸为基础的水凝胶作为控制Senexin a的递送系统。

Panita Maturavongsadit, Weiwei Wu, Jingyu Fan, Igor B Roninson, Taixing Cui, Qian Wang, Tc, Qw, Pm, Fj, Ww, Pm, Tc, Qw, Pm, Fj, Tc, Qw
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引用次数: 1

摘要

血管周围输送治疗药物对抗闭塞性血管重构的既定病因对静脉移植失败有很大的治疗潜力。然而,实验测试的血管周围药物输送系统尚未转化为临床实践。在这项研究中,我们建立了一种新的策略,局部和可持续地递送周期蛋白依赖性激酶8/19抑制剂Senexin a (SenA),这是一种新兴的治疗闭塞性血管疾病的候选药物,使用石墨烯-杂化透明质酸为基础的水凝胶。我们展示了一种通过利用氧化石墨烯纳米片与SenA非共价相互作用来容纳SenA的透明质酸基水凝胶的方法。所得到的水凝胶可以在21天内持续释放SenA,并且释放动力学可调。体外实验也表明水凝胶具有生物相容性。这种新型的氧化石墨烯透明质酸水凝胶作为治疗血管闭塞性疾病(如静脉移植衰竭)的血管周围药物递送系统具有乐观的前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Graphene-incorporated hyaluronic acid-based hydrogel as a controlled Senexin A delivery system.

Graphene-incorporated hyaluronic acid-based hydrogel as a controlled Senexin A delivery system.

Graphene-incorporated hyaluronic acid-based hydrogel as a controlled Senexin A delivery system.

Graphene-incorporated hyaluronic acid-based hydrogel as a controlled Senexin A delivery system.

Perivascular delivery of therapeutic agents against established aetiologies for occlusive vascular remodelling has great therapeutic potential for vein graft failure. However, none of the perivascular drug delivery systems tested experimentally have been translated into clinical practice. In this study, we established a novel strategy to locally and sustainably deliver the cyclin-dependent kinase 8/19 inhibitor Senexin A (SenA), an emerging drug candidate to treat occlusive vascular disease, using graphene oxide-hybridised hyaluronic acid-based hydrogels. We demonstrated an approach to accommodate SenA in hyaluronic acid-based hydrogels through utilising graphene oxide nanosheets allowing for non-covalent interaction with SenA. The resulting hydrogels produced sustained delivery of SenA over 21 days with tunable release kinetics. In vitro assays also demonstrated that the hydrogels were biocompatible. This novel graphene oxide-incorporated hyaluronic acid hydrogel offers an optimistic outlook as a perivascular drug delivery system for treating occlusive vascular diseases, such as vein graft failure.

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CiteScore
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