皮肤替代品在刺激内皮细胞发芽方面比真皮或表皮替代品更有效。

BMC biomedical engineering Pub Date : 2019-07-17 eCollection Date: 2019-01-01 DOI:10.1186/s42490-019-0018-8
Hanneke N Monsuur, Ester M Weijers, Susan Gibbs, Lenie J van den Broek
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引用次数: 2

摘要

背景:治疗抵抗性溃疡是指长时间保持开放的伤口,通常由慢性静脉疾病、长期压力或糖尿病引起。对于慢性伤口的愈合,通过新生血管的新生来激活惰性伤口床是非常重要的。常规疗法的替代治疗选择是使用皮肤替代品:真皮(DS),表皮(ES)或双层皮肤替代品(SS)。本研究的目的是确定自体SS、ES和DS对内皮细胞增殖、迁移和血管生成萌生成纤维蛋白水凝胶的作用模式。结果:SS由一个完全分化的表皮组成,表皮扩张在脱细胞供体真皮(AD)上,该真皮已被成纤维细胞重新填充。DS与SS结构相同,但没有表皮;ES与SS结构相同,但没有成纤维细胞。作为对照,自始至终使用AD。结果表明,双层SS是诱导内皮细胞迁移和发芽的最有效替代物。真皮和表皮间的相互作用导致VEGF和uPAR对发芽的诱导作用最强。通过VEGF和uPAR, ES比DS更能刺激发芽。DS介导的微诱导发芽不是由VEGF介导的,而是部分通过uPAR刺激的。结论:这项体外研究支持了我们的临床观察,即双层SS是一种强大的血管生成刺激剂,因此有可能使惰性伤口床恢复活力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Skin substitutes are more potent than dermal or epidermal substitutes in stimulating endothelial cell sprouting.

Background: Therapy resistant ulcers are wounds that remain open for a long time period and often arise from chronic venous disease, prolonged pressure or diabetes. For healing of chronic wounds, revitalization of the inert wound bed, which is achieved by angiogenic sprouting of new blood vessels is of great importance. An alternative treatment option to conventional therapies is the use of skin substitutes: dermal (DS), epidermal (ES) or bi-layered skin substitutes (SS). The aim of this study was to determine the mode of action of an autologous SS, ES and DS with regards to endothelial cell proliferation, migration and angiogenic sprouting into a fibrin hydrogel.

Results: SS consists of a fully differentiated epidermis expanding over the acellular donor dermis (AD) which has become repopulated with fibroblasts. DS is the same construct as SS but without the epidermis and ES is the same construct as SS but without the fibroblasts. As a control, AD was used throughout. It was found that the bi-layered SS was the most potent substitute in inducing migration and sprouting of endothelial cells. The cross talk between dermis and epidermis resulted in the strongest induction of sprouting via VEGF and uPAR. ES stimulated sprouting more than DS again via VEGF and uPAR. The slight induction of sprouting mediated by DS was not mediated by VEGF, but was in part stimulated through uPAR.

Conclusion: This in vitro study supports our clinical observations that a bi-layered SS is a strong stimulator of angiogenesis and therefore has the potential to revitalize an inert wound bed.

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