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Angiogenesis in the skin of SHARPIN-deficient mice with chronic proliferative dermatitis

机译:SHARPIN缺陷型慢性增生性皮炎小鼠皮肤中的血管生成

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Angiogenesis is a common feature of pathological processes including wound healing, tumor formation, and chronic inflammation. Chronic inflammation can also be associated with dilation or proliferation of lymph vessels. We examined blood vessels and lymphatics and the expression of pro- and anti-angiogenic genes in the skin of SHARPIN-deficient mice which spontaneously develop a chronic proliferative dermatitis (cpdm). The number of blood vessels in the dermis of cpdm mice increased with age as the inflammation progressed. Lymphatics identified by labeling for LYVE1 and podoplanin were moderately dilated, but they were not increased in number. The expression of proangiogenic Vegfa, Flt1 and anti-angiogenic Sema3a mRNA was increased. VEGFA was primarily localized in keratinocytes of cpdm skin. There was also increased expression of Ece1 and Pdpn mRNA. Podoplanin was restricted to lymphatic endothelial cells in normal skin, but fibroblasts in cpdm skin also reacted with anti-podoplanin antibodies indicating that they were activated. The expression of other angiogenic and lymphangiogenic factors was not altered or decreased. These results indicate that cpdm mice may be a useful model to study the pathogenesis of angiogenesis in chronic inflammation. (C) 2016 Elsevier Inc. All rights reserved.
机译:血管生成是包括伤口愈合,肿瘤形成和慢性炎症在内的病理过程的共同特征。慢性炎症也可能与淋巴管扩张或增生有关。我们检查了SHARPIN缺陷小鼠皮肤中的血管和淋巴管以及促血管生成基因和抗血管生成基因的表达,这些基因自发发展为慢性增生性皮炎(cpdm)。随着炎症的发展,cpdm小鼠真皮中的血管数量随着年龄的增长而增加。通过标记LYVE1和Podoplanin鉴定的淋巴瘤被中等程度地扩张,但数量并未增加。促血管生成的Vegfa,Flt1和抗血管生成的Sema3a mRNA的表达增加。 VEGFA主要位于cpdm皮肤的角质形成细胞中。 Ece1和Pdpn mRNA的表达也增加。 Podoplanin限于正常皮肤中的淋巴内皮细胞,但是cpdm皮肤中的成纤维细胞也与抗podoplanin抗体反应,表明它们已被激活。其他血管生成和淋巴血管生成因子的表达未改变或降低。这些结果表明,cpdm小鼠可能是研究慢性炎症中血管生成的发病机制的有用模型。 (C)2016 Elsevier Inc.保留所有权利。

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