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首页> 外文期刊>BMC Cancer >Elevated expression of VEGFR-3 in lymphatic endothelial cells from lymphangiomas
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Elevated expression of VEGFR-3 in lymphatic endothelial cells from lymphangiomas

机译:淋巴管瘤的淋巴管内皮细胞中VEGFR-3的表达升高

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Background Lymphangiomas are neoplasias of childhood. Their etiology is unknown and a causal therapy does not exist. The recent discovery of highly specific markers for lymphatic endothelial cells (LECs) has permitted their isolation and characterization, but expression levels and stability of molecular markers on LECs from healthy and lymphangioma tissues have not been studied yet. We addressed this problem by profiling LECs from normal dermis and two children suffering from lymphangioma, and also compared them with blood endothelial cells (BECs) from umbilical vein, aorta and myometrial microvessels. Methods Lymphangioma tissue samples were obtained from two young patients suffering from lymphangioma in the axillary and upper arm region. Initially isolated with anti-CD31 (PECAM-1) antibodies, the cells were separated by FACS sorting and magnetic beads using anti-podoplanin and/or LYVE-1 antibodies. Characterization was performed by FACS analysis, immunofluorescence staining, ELISA and micro-array gene analysis. Results LECs from foreskin and lymphangioma had an almost identical pattern of lymphendothelial markers such as podoplanin, Prox1, reelin, cMaf and integrin-α1 and -α9. However, LYVE-1 was down-regulated and VEGFR-2 and R-3 were up-regulated in lymphangiomas. Prox1 was constantly expressed in LECs but not in any of the BECs. Conclusion LECs from different sources express slightly variable molecular markers, but can always be distinguished from BECs by their Prox1 expression. High levels of VEGFR-3 and -2 seem to contribute to the etiology of lymphangiomas.
机译:背景淋巴管瘤是儿童时期的肿瘤。他们的病因未知,不存在因果疗法。淋巴管内皮细胞(LEC)的高度特异性标记物的最新发现允许对其进行分离和表征,但是尚未研究健康和淋巴管瘤组织的LEC上分子标记物的表达水平和稳定性。我们通过分析正常真皮和两个患淋巴管瘤的儿童的LEC来解决这个问题,并将它们与脐静脉,主动脉和子宫肌层微血管的血管内皮细胞(BEC)进行比较。方法从两名年轻腋窝和上臂淋巴管瘤患者中获取淋巴管瘤组织样本。最初用抗CD31(PECAM-1)抗体分离,然后使用抗Podoplanin和/或LYVE-1抗体通过FACS分选和磁珠分离细胞。通过FACS分析,免疫荧光染色,ELISA和微阵列基因分析进行表征。结果包皮和淋巴管瘤的LEC具有几乎相同的淋巴内皮标记物模式,如podoplanin,Prox1,reelin,cMaf和整联蛋白-α1和-α9。然而,淋巴管瘤中LYVE-1被下调,而VEGFR-2和R-3被上调。 Prox1在LEC中不断表达,但在任何BEC中都不表达。结论来自不同来源的LEC表达的分子标记略有变化,但始终可以通过Prox1表达与BEC区别。高水平的VEGFR-3和-2似乎与淋巴管瘤的病因有关。

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