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白细胞介素-7对人内皮细胞淋巴管生成特性的影响。

The effects of interleukin-7 on the lymphangiogenic properties of human endothelial cells.

作者信息

Al-Rawi Mahir A A, Watkins Gareth, Mansel Robert E, Jiang Wen G

机构信息

Department of Surgery, University of Wales College of Medicine, Heath Park, Cardiff CF14 XN, UK.

出版信息

Int J Oncol. 2005 Sep;27(3):721-30.

PMID:16077922
Abstract

Lymphangiogenesis (growth of new lymphatic vessels) is thought to play an important role in cancer lymphatic spread to the regional lymph nodes. However, the molecular pathways involved in lymphangiogenesis and their regulation are still unclear. Recently, there has been a significant advance in the studies of the lymphatic system and lymphangiogenesis as several novel specific lymphatic markers are discovered. Here, the effects of several cytokines on the lymphatic expression of human endothelial cells were studied. Amongst these cytokines, interleukin-7 (IL-7) was found to have significant impact on the lymphatic expression as it induced the expression of podoplanin, prox-1 and LYVE-1 in endothelial cells. Furthermore, IL-7 enhanced endothelial cell growth, migration and generation of lymphatic tubules in vitro via upregulating the expression of the lymphangiogenic growth factor and vascular endothelial growth factor-D. The specificity of these effects of IL-7 was confirmed using blocking anti-bodies and ribozyme transgene technology. These effects of IL-7 were totally abolished when IL-7R null endothelial cell mutants were used. IL-7 activated its transmembrane receptor, IL-7R, on endothelial cells, as well as its downstream signalling intermediates, Jak-1, Jak-3, PI3-K and Stat-5. Selective inhibition of these intermediates using specific inhibitors showed that IL-7 induced the afore-mentioned effects via a Wortmannin sensitive pathway. Collectively, these results demonstrate, for the first time, that IL-7 is a lymphangiogenic growth factor by inducing the lymphangiogenic properties of endothelial cells. This might have a significant impact on the lymphatic spread of solid tumours. Furthermore, interruption of IL-7 signalling might provide an attractive therapeutic option in cancer lymphatic metastasis.

摘要

淋巴管生成(新淋巴管的生长)被认为在癌症向区域淋巴结的淋巴转移中起重要作用。然而,参与淋巴管生成的分子途径及其调控仍不清楚。最近,随着几种新型特异性淋巴管标志物的发现,淋巴管系统和淋巴管生成的研究取得了重大进展。在此,研究了几种细胞因子对人内皮细胞淋巴管表达的影响。在这些细胞因子中,发现白细胞介素-7(IL-7)对淋巴管表达有显著影响,因为它能诱导内皮细胞中血小板反应蛋白-1、prox-1和淋巴管内皮透明质酸受体-1(LYVE-1)的表达。此外,IL-7通过上调淋巴管生成生长因子和血管内皮生长因子-D的表达,在体外增强内皮细胞生长、迁移和淋巴管生成。使用阻断抗体和核酶转基因技术证实了IL-7这些作用的特异性。当使用IL-7R基因缺失的内皮细胞突变体时,IL-7的这些作用完全消失。IL-7激活内皮细胞上的跨膜受体IL-7R及其下游信号中间体Jak-1、Jak-3、磷脂酰肌醇-3激酶(PI3-K)和信号转导子和转录激活子-5(Stat-5)。使用特异性抑制剂对这些中间体进行选择性抑制表明,IL-7通过一种渥曼青霉素敏感途径诱导上述作用。总的来说,这些结果首次证明,IL-7通过诱导内皮细胞的淋巴管生成特性而成为一种淋巴管生成生长因子。这可能对实体瘤的淋巴转移有重大影响。此外,中断IL-7信号传导可能为癌症淋巴转移提供一种有吸引力的治疗选择。

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