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白细胞介素-1刺激的白细胞介素-8和生长相关癌基因-α的分泌表明,在人表皮筏培养物中角质形成细胞的生长大大增强。

Interleukin-1-stimulated secretion of interleukin-8 and growth-related oncogene-alpha demonstrates greatly enhanced keratinocyte growth in human raft cultured epidermis.

作者信息

Steude Judith, Kulke Reinhard, Christophers Enno

机构信息

Institute of Immunology, University of Kiel, Michaelisstr. 5, 24105 Kiel, Germany.

出版信息

J Invest Dermatol. 2002 Dec;119(6):1254-60. doi: 10.1046/j.1523-1747.2002.19616.x.

Abstract

The CXC chemokines, interleukin-8 and growth-related oncogenealpha, are known to play a prominent part in wound healing as well as inflammatory skin disorders, including psoriasis. Both chemokines are potent neutrophil activators and were discussed as potential stimuli in keratinocyte growth. We examined the action of growth-related oncogene alpha and interleukin-8 in organotypic raft culture, which resembles in vivo skin in several respects. Addition of growth-related oncogene alpha and interleukin-8 resulted in a time- and concentration-dependent epidermal hyperproliferation in organotypic cultures. In cryostat sections an increased number of epidermal layers as well as significantly elevated number of Ki-67-stained keratinocytes indicate marked hyperproliferation with no evidence for the reduction of apoptotic cells. Terminal differentiation was shown to proceed in a regular fashion with formation of a cornified layer and the expression of suprabasal keratins in addition to the presence of differentiation markers. Interleukin-8-mediated hyperproliferation was inhibited by a blocking human monoclonal antibody. To demonstrate a specific receptor-mediated action of growth-related oncogene and interleukin-8, we used a CXC receptor 2 monoclonal antibody or a CXC receptor 2 selective nonpeptide antagonist, both of which lead to inhibition of interleukin-8-mediated hyperproliferation. Interleukin-1alpha caused induction of interleukin-8 and growth-related oncogene alpha mRNA as well as marked epidermal hyperproliferation. The interleukin-1alpha-mediated hyperproliferation was markedly reduced by both the interleukin-8-specific antibody and the CXC receptor 2 antagonist, indicating close correlation between the interleukin-8/CXC receptor 2 pathway and interleukin-1-induced keratinocyte growth stimulation. Our data indicate that interleukin-1 induces overexpression of interleukin-8 and growth-related oncogene alpha in human keratinocytes. These changes correlate with characteristic functional alterations of the epidermis as observed in psoriasis and wound healing.

摘要

CXC趋化因子、白细胞介素-8和生长相关癌基因α在伤口愈合以及包括银屑病在内的炎症性皮肤病中发挥着重要作用。这两种趋化因子都是有效的中性粒细胞激活剂,并且被认为是角质形成细胞生长的潜在刺激因素。我们在器官型筏式培养中研究了生长相关癌基因α和白细胞介素-8的作用,该培养在多个方面类似于体内皮肤。添加生长相关癌基因α和白细胞介素-8导致器官型培养中出现时间和浓度依赖性的表皮过度增殖。在冷冻切片中,表皮层数增加以及Ki-67染色的角质形成细胞数量显著升高表明存在明显的过度增殖,且没有凋亡细胞减少的证据。终末分化显示以正常方式进行,形成了角质层,除了存在分化标志物外,还表达了基底层以上的角蛋白。白细胞介素-8介导的过度增殖被一种阻断性人单克隆抗体抑制。为了证明生长相关癌基因和白细胞介素-8的特异性受体介导作用,我们使用了一种CXC受体2单克隆抗体或一种CXC受体2选择性非肽拮抗剂,两者均导致白细胞介素-8介导的过度增殖受到抑制。白细胞介素-1α导致白细胞介素-8和生长相关癌基因α mRNA的诱导以及明显的表皮过度增殖。白细胞介素-8特异性抗体和CXC受体2拮抗剂均显著降低了白细胞介素-1α介导的过度增殖,表明白细胞介素-8/CXC受体2途径与白细胞介素-1诱导的角质形成细胞生长刺激之间密切相关。我们的数据表明,白细胞介素-1诱导人角质形成细胞中白细胞介素-8和生长相关癌基因α的过表达。这些变化与银屑病和伤口愈合中观察到的表皮特征性功能改变相关。

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