首页> 外文期刊>Experimental Biology and Medicine: Journal of the Society for Experimental Biology and Medicine >Exogenous administration of substance p enhances wound healing in a novel skin-injury model.
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Exogenous administration of substance p enhances wound healing in a novel skin-injury model.

机译:在新的皮肤损伤模型中,物质p的外源给药可促进伤口愈合。

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摘要

Soft tissue injury accounts for approximately 44% of all wounds in both the military and civilian populations. Following injury to soft tissue, Substance P (SP) and other neuropeptides are released by cutaneous neurons and modulate the function of immunocompetent and inflammatory cells, as well as epithelial and endothelial cells. The interaction between these components of the nervous system and multiple target cells affecting cutaneous repair is of increasing interest. In this report, we describe the effects of SP on wound repair in a novel, laser-induced, skin-wound model. Gross and histologic examination of laser-induced injury revealed that exogenously administered SP affects wound healing via neurite outgrowth, in addition to adhesion molecule and neurokinin-1 receptor involvement in vivo. All SP effects were decreased by pretreatment with Spantide II, an SP antagonist. The elucidation of SP-mediating mechanisms is crucial to firmly establishing the involvement and interaction of the peripheral nervous system and the immune system in cutaneous repair. Findings presented here suggest that SP participates in the complex network of mediators involved in cutaneous inflammation and wound healing.
机译:在军队和平民中,软组织损伤约占所有伤口的44%。在软组织受到损伤之后,物质P(SP)和其他神经肽会被皮肤神经元释放,并调节免疫功能和炎症细胞以及上皮和内皮细胞的功能。神经系统的这些组件与影响皮肤修复的多个靶细胞之间的相互作用越来越引起人们的关注。在这份报告中,我们描述了SP在新型激光诱导皮肤伤口模型中对伤口修复的影响。激光诱导损伤的大体和组织学检查显示,外源性SP不仅通过体内粘附分子和Neurokinin-1受体参与,还通过神经突向外生长影响伤口愈合。通过用SP拮抗剂Spantide II预处理,所有SP效果均降低。对SP介导机制的阐明对于在皮肤修复中牢固地建立周围神经系统和免疫系统的参与和相互作用至关重要。此处发现的结果表明SP参与了涉及皮肤炎症和伤口愈合的复杂介体网络。

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