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新型全层三维非角化黏液膜模型在创伤愈合中的药理学研究。

Novel Human Full-Thickness Three-Dimensional Nonkeratinized Mucous Membrane Model for Pharmacological Studies in Wound Healing.

机构信息

Department of Dermatology and Allergology, Medical Faculty, RWTH Aachen University, Aachen, Germany,

Department of Dermatology and Allergology, Medical Faculty, RWTH Aachen University, Aachen, Germany.

出版信息

Skin Pharmacol Physiol. 2019;32(5):265-274. doi: 10.1159/000501733. Epub 2019 Jul 8.

Abstract

INTRODUCTION

Efforts are increasingly aiming to develop in vitro models that can provide effective alternatives to in vivo experiments. The main aim of this study was the establishment of an in vitro model of the nonkeratinized mucous membrane that can be used as a standardized tool to evaluate biological and therapeutic effects of pharmaceuticals for mucosal wound healing.

METHODS

We established a full-thickness in vitro model of the nonkeratinized mucous membrane. While histological examination was performed to assess morphological characteristics, we utilized gene expression profiling using microarray and qRT-PCR analyses to identify molecular effects of treatment with a dexpanthenol-containing ointment after laser wounding.

RESULTS

Performing histological and immunofluorescence analyses we proved that our model mimics the two distinctive layers of the mucous membrane - the stratified squamous epithelium and the lamina propria. We used this model to investigate molecular effects of a dexpanthenol-containing ointment that is commonly used for the wound treatment of mucous membranes. For that purpose, our model exhibits a unique feature in that dexpanthenol and proliferation-enhancing additives that may interfere with our studies are not required for the maintenance of the model culture. After setting standardized lesions with a nonsequential fractional ultrapulsed CO2 laser, topical treatment with the dexpanthenol-containing ointment enhanced wound closure in the model compared to placebo and untreated controls. Furthermore, microarray analysis revealed that the treatment of the laser-wounded model with the dexpanthenol-containing ointment evoked an upregulated expression of various genes related to accelerated wound healing.

CONCLUSION

Overall, we verified that this novel mucous membrane model can be utilized in future to monitor ex vivo effects of various topical therapies on mucosa morphology, physiology, and gene expression. Our findings confirm the potential of the model as an in vitro tool for the replacement of pharmacological in vivo studies regarding mucosal wound healing.

摘要

简介

目前,人们越来越致力于开发能够替代体内实验的体外模型。本研究的主要目的是建立一种可用于评估黏膜创伤愈合药物生物学和治疗效果的非角质化黏膜体外模型。

方法

我们建立了一种非角质化黏膜的全层体外模型。在进行组织学检查以评估形态特征的同时,我们还利用微阵列和 qRT-PCR 分析进行基因表达谱分析,以确定含泛醇软膏治疗激光创伤后的分子效应。

结果

通过组织学和免疫荧光分析,我们证明了我们的模型模拟了黏膜的两个独特层 - 复层鳞状上皮和固有层。我们使用该模型研究了一种常用的黏膜创伤治疗含泛醇软膏的分子效应。为此,我们的模型具有一个独特的特征,即不需要泛醇和可能干扰我们研究的增殖增强添加剂来维持模型培养。用非顺序分数超脉冲 CO2 激光设置标准化损伤后,与安慰剂和未处理对照相比,局部应用含泛醇软膏可增强模型中的伤口闭合。此外,微阵列分析显示,用含泛醇软膏治疗激光创伤模型可上调与加速伤口愈合相关的各种基因的表达。

结论

总的来说,我们验证了这种新型黏膜模型可用于监测各种局部治疗对黏膜形态、生理学和基因表达的体外效应。我们的研究结果证实了该模型作为一种替代黏膜创伤愈合的体内药理学研究的体外工具的潜力。

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