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A mechanics approach to the study of pressure sensitive adhesives and human skin for transdermal drug delivery applications.

机译:一种力学方法,用于研究透皮给药应用的压敏粘合剂和人体皮肤。

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Transdermal drug delivery is an alternative approach to the systemic delivery of pharmaceuticals where drugs are administered through the skin and absorbed percutaneously. This method of delivery offers several advantages over more traditional routes; most notably, the avoidance of the fast-pass metabolism of the liver and gut, the ability to offer controlled release rates, and the possibility for novel devices. Pressure sensitive adhesives (PSAs) are used to bond transdermal drug delivery devices to the skin because of their good initial and long-term adhesion, clean removability, and skin and drug compatibility. However, an understanding of the mechanics of adhesion to the dermal layer, together with quantitative and reproducible test methods for measuring adhesion, have been lacking. This study utilizes a mechanics-based approach to quantify the interfacial adhesion of PSAs bonded to selected substrates, including human dermal tissue.; The delamination of PSA layers is associated with cavitation in the PSA followed by the formation of an extensive cohesive zone behind the debond tip. A quantitative metrology was developed to assess the adhesion and delamination of PSAs, such that it could be possible to easily distinguish between the adhesive characteristics of different PSA compositions and to provide a quantitative basis from which the reliability of adhesive layers bonded to substrates could be studied. A mechanics-based model was also developed to predict debonding in terms of the relevant energy dissipation mechanisms active during this process.; As failure of transdermal devices may occur cohesively within the PSA layer, adhesively at the interface between the PSA and the skin, or cohesively between the corneocytes that comprise the outermost layer of the skin, it was also necessary to explore the mechanical and fracture properties of human skin. The out-of-plane delamination of corneocytes was studied by determining the strain energy release rate during debonding of cantilever-beam specimens containing thin layers of human dermal tissue at their midline. Finally, the interfacial adhesion of PSAs bonded to human skin was studied and the mechanics model that was developed for PSA failure was extended to provide the capability for in vivo reliability predictions for transdermal systems bonded to human skin.
机译:透皮药物递送是药物全身递送的替代方法,其中药物通过皮肤施用并经皮吸收。与更传统的路线相比,这种传递方式具有许多优势。最值得注意的是,避免了肝脏和肠道的快速通过代谢,提供控制释放速率的能力以及新型装置的可能性。压敏胶(PSA)由于其良好的初始和长期粘合性,清洁的可去除性以及皮肤和药物的相容性而用于将透皮药物传递装置粘合到皮肤上。然而,缺乏对与真皮层的粘附力的力学以及用于测量粘附力的定量和可再现的测试方法的了解。这项研究利用了一种基于力学的方法来量化PSA与所选基质(包括人类皮肤组织)的界面粘合力。 PSA层的分层与PSA中的空化作用有关,随后在脱胶尖端后面形成了一个宽大的内聚区。开发了一种定量计量学,以评估PSA的粘附性和分层性,从而可以轻松地区分不同PSA组合物的粘合特性,并提供定量基础,从中可以研究粘合到基材的粘合剂层的可靠性。还建立了基于力学的模型,以根据在此过程中活跃的相关能量耗散机制来预测脱胶。由于透皮设备的故障可能会在PSA层内凝结,在PSA与皮肤之间的界面处凝结或在构成皮肤最外层的角质细胞之间凝结发生,因此有必要探索皮肤的机械和断裂特性人类的皮肤。通过确定在中线处包含人类皮肤组织薄层的悬臂梁样品脱粘过程中的应变能释放速率,研究了角质细胞的面外分层。最后,研究了粘合到人体皮肤的PSA的界面粘附力,并扩展了为PSA失败而开发的力学模型,从而为粘合到人体皮肤的透皮系统提供了 in vivo 可靠性预测的功能。

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