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芥子气对体外培养的人体皮肤模型的微囊泡化作用。

Microvesicating effects of sulfur mustard on an in vitro human skin model.

作者信息

Hayden Patrick J, Petrali John P, Stolper Gina, Hamilton Tracey A, Jackson George R, Wertz Philip W, Ito Susumu, Smith William J, Klausner Mitchell

机构信息

MatTek Corp., 200 Homer Avenue, Ashland, MA 01721, USA.

出版信息

Toxicol In Vitro. 2009 Oct;23(7):1396-405. doi: 10.1016/j.tiv.2009.07.021. Epub 2009 Jul 18.

Abstract

Bis-(beta-chloroethyl) sulfide (SM) is a potent skin vesicant previously used for chemical warfare. Progress in determination of the mechanistic basis of SM pathology, and development of prophylactic and/or therapeutic countermeasures to SM exposure has been hampered by lack of physiologically relevant models of human skin. The current work evaluated a newly developed tissue engineered full-thickness human skin model in a completely in vitro approach to investigation of SM-induced dermal pathology. The model was first characterized with regard to overall morphology, lipid composition, basement membrane (BM) composition and ultrastructural features that are important targets of SM pathologic activity. Well-developed BM ultrastructural features were observed at the dermal-epidermal junction (DEJ), thus demonstrating successful resolution of a primary deficiency of models previously evaluated for SM studies. Studies were then conducted to evaluate histopathological effects of SM on the model. Good replication of in vivo effects was observed, including apoptosis of basal keratinocytes (KC) and microblister formation at the DEJ. Tissue engineered skin models with well-developed basement membrane structures thus appear to be useful tools for in vitro mechanistic studies of SM vesicant activity and development of preventive/therapeutic approaches for SM pathology.

摘要

双(β-氯乙基)硫化物(SM)是一种强效皮肤发泡剂,曾用于化学战。由于缺乏与人类皮肤生理相关的模型,在确定SM病理学的机制基础以及开发针对SM暴露的预防和/或治疗对策方面的进展受到了阻碍。当前的工作采用完全体外的方法,评估了一种新开发的组织工程化全层人类皮肤模型,以研究SM诱导的皮肤病理学。该模型首先在整体形态、脂质组成、基底膜(BM)组成以及超微结构特征方面进行了表征,这些都是SM病理活性的重要靶点。在真皮-表皮交界处(DEJ)观察到发育良好的BM超微结构特征,从而证明成功解决了先前用于SM研究的模型的一个主要缺陷。然后进行研究以评估SM对该模型的组织病理学影响。观察到体内效应的良好重现性,包括基底角质形成细胞(KC)的凋亡以及DEJ处的微水疱形成。因此,具有发育良好的基底膜结构的组织工程皮肤模型似乎是用于SM发泡剂活性体外机制研究以及开发针对SM病理学的预防/治疗方法的有用工具。

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