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一种可灌注血管化全层皮肤模型,可用于潜在的局部和全身应用。

A perfusable vascularized full-thickness skin model for potential topical and systemic applications.

机构信息

L'Oréal Research and Innovation, Aulnay-sous-Bois, France.

Sorbonne Université, Collège Doctoral, F-75005 Paris, France.

出版信息

Biofabrication. 2021 May 14;13(3). doi: 10.1088/1758-5090/abfca8.

Abstract

Vascularization of reconstructed tissues is one of the remaining hurdles to be considered to improve both the functionality and viability of skin grafts and the relevance ofapplications. Our study, therefore, sought to develop a perfusable vascularized full-thickness skin equivalent that comprises a more complex blood vasculature compared to existing models. We combined molding, auto-assembly and microfluidics techniques in order to create a vascularized skin equivalent representing (a) a differentiated epidermis with a physiological organization and correctly expressing K14, K10, Involucrin, TGM1 and Filaggrin, (b) three perfusable vascular channels with angiogenic sprouts stained with VE-Caderin and Collagen IV, (c) an adjacent microvascular network created via vasculogenesis and connected to the sprouting macrovessels. Histological analysis and immunostaining of CD31, Collagen IV, Perlecan and Laminin proved the integrity of vascular constructs. In order to validate the vascularized skin potential of topical and systemic applications, caffeine and minoxidil, two compounds with different chemical properties, were topically applied to measure skin permeability and benzo[a]pyrene pollutant was systemically applied to evaluate systemic delivery. Our results demonstrated that perfusion of skin reconstructs and the presence of a complex vascular plexus resulted in a more predictive and reliable model to assess respectively topical and systemic applications. This model is therefore aimed at furthering drug discovery and improving clinical translation in dermatology.

摘要

血管化是重建组织需要考虑的一个关键问题,这有助于提高皮肤移植物的功能和活力,以及相关应用的相关性。因此,我们的研究旨在开发一种可灌注的全层血管化皮肤等效物,与现有模型相比,它具有更复杂的血管系统。我们结合了成型、自动组装和微流控技术,以创建一种血管化的皮肤等效物,该等效物代表(a)具有生理组织结构且正确表达 K14、K10、内披蛋白、TGM1 和 Filaggrin 的分化表皮,(b)具有血管生成芽且用 VE-Caderin 和 Collagen IV 染色的三个可灌注的血管通道,(c)通过血管生成形成并与发芽的大血管相连的相邻微血管网络。CD31、Collagen IV、Perlecan 和 Laminin 的组织学分析和免疫染色证明了血管结构的完整性。为了验证局部和全身应用的血管化皮肤的潜力,我们局部应用了咖啡因和米诺地尔两种具有不同化学性质的化合物来测量皮肤通透性,并系统应用了苯并[a]芘污染物来评估全身输送。我们的结果表明,皮肤重建的灌注和复杂血管丛的存在导致了一个更具预测性和可靠性的模型,分别用于评估局部和全身应用。因此,该模型旨在促进药物发现并改善皮肤科的临床转化。

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