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VEGF 表达的上调与未治疗硬皮病患者皮肤中 HIF-1α 的积累有关。

Upregulation of VEGF expression is associated with accumulation of HIF-1α in the skin of naïve scleroderma patients.

机构信息

Medical School, University of Thessaly, Larisa, Greece.

出版信息

Mod Rheumatol. 2013 Nov;23(6):1245-8. doi: 10.1007/s10165-012-0787-6. Epub 2012 Oct 25.

DOI:10.1007/s10165-012-0787-6
PMID:23096096
Abstract

Systemic sclerosis is a disease hallmarked by microangiopathy; the enlargement and leakage of skin capillaries in active stages develops into extensive avascular areas, clinically associated with severe tissue hypoxia and the formation of digital ulcers. Vascular endothelial growth factor (VEGF) is upregulated in all stages of the disease, with little effect on efficient neovascularization. The oxygen-regulated α-subunit of hypoxia-inducible transcription factor-1 (HIF-1α) represents a key mechanism involved in the transcriptional regulation of VEGF. The aim of this study is to investigate expression of the oxygen-regulated α-subunit of HIF-1 and VEGF in naïve scleroderma patients. For this purpose, skin biopsies (dorsal hand surface) from scleroderma patients were analyzed and compared with control skin biopsies. Immunoreactivity for VEGF was enhanced in scleroderma patients, in contrast to restricted positive immunostaining in suprabasal keratinocytes observed in normal skin. In a similar fashion, all skin biopsies from scleroderma patients were strongly HIF-1α reactive, compared with rare immunoreactivity observed in normal skin. The pattern was similar in all stages of scleroderma. These observations for the first time directly connect constitutive hypoxia with VEGF upregulation in scleroderma patients. The sequence of events needs to be precisely mapped, and the pro- and antiangiogenic switches which may interfere with efficient tissue neovascularization identified, in order to provide meaningful therapeutic strategies.

摘要

系统性硬化症是一种以微血管病变为特征的疾病;在活动期,皮肤毛细血管扩张和渗漏会发展为广泛的无血管区域,临床上与严重的组织缺氧和形成手指溃疡有关。血管内皮生长因子(VEGF)在疾病的所有阶段都上调,但对有效的新血管生成影响不大。缺氧诱导因子-1(HIF-1)的氧调节α亚基是参与 VEGF 转录调节的关键机制之一。本研究旨在研究幼稚型硬皮病患者中 HIF-1 的氧调节α亚基和 VEGF 的表达。为此,分析了硬皮病患者的皮肤活检(手背)并与对照皮肤活检进行了比较。与正常皮肤中观察到的基底上层角质形成细胞的有限阳性免疫染色相比,VEGF 的免疫反应性在硬皮病患者中增强。同样,与正常皮肤中观察到的罕见免疫反应性相比,所有硬皮病患者的皮肤活检均强烈反应 HIF-1α。这种模式在硬皮病的所有阶段都是相似的。这些观察结果首次直接将持续缺氧与硬皮病患者中 VEGF 的上调联系起来。需要精确绘制事件序列,并确定可能干扰有效组织新血管生成的促血管生成和抗血管生成开关,以提供有意义的治疗策略。

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