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Smart Microneedles with Porous Polymer Coatings for pH-Responsive Drug Delivery

机译:带有多孔聚合物涂层的智能微针用于pH响应药物输送

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摘要

This work demonstrates a simple approach for coating a porous polymer layer on stainless-steel (SS) microneedles characterized by a pH-responsive formulation for self-regulated drug delivery. For many drug-delivery applications, the release of therapeutic agents in an acidic microenvironment is desirable. Acid-sensitive polymers and hydrogels were extensively explored, but easily prepared polymeric microcarriers that combine acid sensitivity and biodegradability are rare. Here, we describe a simple and robust method of coating a porous polymer layer on SS microneedles (MNs) that release a model drug (lidocaine) in a pH-responsive fashion. It was constructed by packing the model drug and a pH-sensitive component (sodium bicarbonate) into the pores of the polymer layer. When this acid-sensitive formulation was exposed to the acidic microenvironment, the consequent reaction of protons (H ) with sodium bicarbonate (NaHCO ) yielded CO . This effect generated pressure inside the pores of the coating and ruptured the thin polymer membrane, thereby releasing the encapsulated drug. Scanning electron micrographs showed that the pH-sensitive porous polymer-coated MNs exposed to phosphate-buffered saline (PBS) at pH 7.4 were characterized by closed pores. However, MNs exposed to PBS at pH 5.5 consisted of open pores and the thin membrane burst. The in vitro studies demonstrated the pH sensitivity of the drug release from porous polymer-coated MNs. Negligible release was observed for MNs in receiving media at pH 7.4. In contrast, significant release occurred when the MNs were exposed to acidic conditions (pH 5.5). Additionally, comparable results were obtained for drug release in vitro in porcine skin and in PBS. This revealed that our developed pH-responsive porous polymer-coated MNs could potentially be used for the controlled release of drug formulations in an acidic environment. Moreover, the stimuli-responsive drug carriers will enable on-demand controlled release profiles that may enhance therapeutic effectiveness and reduce systemic toxicity.
机译:这项工作展示了一种简单的方法,可以在不锈钢(SS)微针上涂覆多孔聚合物层,其特征在于具有pH响应配方,可自我调节药物输送。对于许多药物递送应用,期望在酸性微环境中释放治疗剂。对酸敏感性聚合物和水凝胶进行了广泛的探索,但结合酸敏感性和生物降解性的易于制备的聚合物微载体很少见。在这里,我们描述了一种在SS微针(MNs)上涂覆多孔聚合物层的简单而可靠的方法,该方法以pH响应方式释放模型药物(利多卡因)。它是通过将模型药物和pH敏感成分(碳酸氢钠)填充到聚合物层的孔中而构建的。当这种对酸敏感的制剂暴露于酸性微环境时,质子(H)与碳酸氢钠(NaHCO)的随后反应生成了CO。这种作用在涂层的孔内产生压力并使聚合物薄膜破裂,从而释放出包封的药物。扫描电子显微镜照片显示,暴露于pH 7.4的磷酸盐缓冲盐水(PBS)的pH敏感的多孔聚合物涂层MNs具有封闭的孔。但是,在pH 5.5下暴露于PBS的MN由开孔和薄膜破裂组成。体外研究表明药物从多孔聚合物包衣的MNs释放的pH敏感性。在pH 7.4的接收介质中,MN的释放可忽略不计。相反,当MNs暴露于酸性条件(pH 5.5)时,会发生大量释放。另外,获得了在猪皮肤和PBS中体外药物释放的可比结果。这表明我们开发的pH响应多孔聚合物涂层的MNs可以潜在地用于酸性环境中药物制剂的控释。此外,刺激反应性药物载体将实现按需控制释放,从而可以增强治疗效果并降低全身毒性。

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