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血管内皮生长因子与信号素3A的比值升高是人类脑膜瘤的不良预后因素。

Increased ratio of vascular endothelial growth factor to semaphorin3A is a negative prognostic factor in human meningiomas.

作者信息

Barresi Valeria, Tuccari Giovanni

机构信息

Department of Human Pathology, University of Messina, Messina, Italy.

出版信息

Neuropathology. 2010 Oct;30(5):537-46. doi: 10.1111/j.1440-1789.2010.01105.x.

DOI:10.1111/j.1440-1789.2010.01105.x
PMID:20337947
Abstract

Semaphorin3A (SEMA3A) is an anti-angiogenic factor which is expressed in human meningiomas in association with low microvessel density (MVD). It competes with vascular endothelial growth factor (VEGF) for receptor neuropilin-1 (NRP-1). The ratio between VEGF and SEMA3A has been recently demonstrated to regulate neo-angiogenesis, proliferation and progression of tumors. To clarify the involvement of these proteins in the above-mentioned phenomena, we analyzed the immunohistochemical expression of SEMA3A, VEGF and NRP-1 and their correlation with MVD in a series of 48 cases of meningioma with different histotype and histological grade. SEMA3A and VEGF expression was encountered in about half the cases, although at different levels. NRP-1 staining was evidenced in the vessels within all but two tumors and in the neoplastic cells of 18/48 meningiomas. A negative significant correlation emerged between SEMA3A amount and MVD; on the other hand, high VEGF levels appeared to be significantly associated with high MVD. A high VEGF/SEMA3A was significantly associated with high histological grade, proliferation index and MVD as well as with a higher recurrence rate of the meningiomas. Present data suggest that the balance between the expression of the pro-angiogenic factor VEGF and the anti-angiogenic SEMA3A may be involved in the regulation of neo-angiogenesis and proliferation in meningiomas, representing also a predictor of recurrences in these tumors. Further validation of our results may open the way for the use of drugs targeting not only VEGF, but also NRP-1 and SEMA3A to prevent recurrences of meningiomas.

摘要

信号素3A(SEMA3A)是一种抗血管生成因子,在人类脑膜瘤中表达,与低微血管密度(MVD)相关。它与血管内皮生长因子(VEGF)竞争受体神经纤毛蛋白-1(NRP-1)。最近已证明VEGF与SEMA3A之间的比例可调节肿瘤的新生血管生成、增殖和进展。为了阐明这些蛋白质在上述现象中的作用,我们分析了48例不同组织学类型和组织学分级的脑膜瘤中SEMA3A、VEGF和NRP-1的免疫组化表达及其与MVD的相关性。约半数病例中可检测到SEMA3A和VEGF表达,尽管表达水平不同。除两例外,所有肿瘤内的血管以及48例脑膜瘤中的18例肿瘤细胞中均有NRP-1染色。SEMA3A含量与MVD之间呈显著负相关;另一方面,高VEGF水平似乎与高MVD显著相关。高VEGF/SEMA3A与高组织学分级、增殖指数和MVD显著相关,也与脑膜瘤的较高复发率相关。目前的数据表明,促血管生成因子VEGF和抗血管生成因子SEMA3A之间的表达平衡可能参与脑膜瘤新生血管生成和增殖的调节,也代表了这些肿瘤复发的一个预测指标。对我们结果的进一步验证可能为使用不仅靶向VEGF,而且靶向NRP-1和SEMA3A的药物来预防脑膜瘤复发开辟道路。

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