Taïeb David, Barlier Anne, Yang Chunzhang, Pertuit Morgane, Tchoghandjian Aurélie, Rochette Claire, Zattara-Canoni Hélène, Figarella-Branger Dominique, Zhuang Zhengping, Pacak Karel, Metellus Philippe
Department of Nuclear Medicine, La Timone University Hospital & CERIMED & Inserm UMR1068 Marseille Cancerology Research Center, Institut Paoli-Calmettes, Aix-Marseille University, 264 RUE Saint-Pierre, 13385, Marseille, France.
Laboratory of Molecular Biology, Conception Hospital & CNRS, CRN2M UMR 7286, Aix-Marseille University, Marseille, France.
J Neurooncol. 2016 Feb;126(3):473-81. doi: 10.1007/s11060-015-1983-y. Epub 2015 Oct 29.
Central nervous system hemangioblastomas (CNS-HBs) occur sporadically or as a component of von Hippel-Lindau-VHL syndrome. CNS-HBs share some molecular similarities with pheochromocytomas/paragangliomas (PPGLs) and renal cell carcinomas (RCCs). Recently, hypoxia-inducible factors, particularly somatic HIF2A mutations, have been found to play an important role in the pathogenesis of PPGLs. Somatic mutations in HIF2A have been reported in PPGLs associated with polycythemia, which have been reported to also be present in patients with RCCs and HBs. However, whether CNS-HBs is associated with the presence of a HIF2A mutation is currently uknown. We analyzed somatic HIF2A and VHL mutations in a series of 28 sporadic CNS-HBs. We also investigated the expression of HIF target proteins and hypoxia-associated factor (HAF). Two sporadic CNS-HBs were found to have somatic HIF2A mutations. One tumor had 2 HIF2A missense mutations, one of which was previously described in a PPGL (c.1121 T>A, F374Y). The second patient had coexistence of somatic truncated mutations (c.1669 C>T, Q557*) in HIF2A together with a VHL mutation. Neither of the two patients had polycythemia at the time of diagnosis. We demonstrate that the novel truncated mutation in HIF2A (Q557*) affects HIF-2α prolyl hydroxylation with its reduced ubiquitination but intact transcriptional activity, resulting in an activating effect. Both CNS-HB samples showed positive expression of VEGFR2/CA9/Glut1 and HAF. Our data support the unique central role of the VHL/HIF-2α signaling pathway in the molecular pathogenesis of CNS-HBs and show for the first time the presence of HIF2A mutations in sporadic HB.
中枢神经系统血管母细胞瘤(CNS-HBs)可散发出现,或作为冯·希佩尔-林道-韦尔综合征(VHL综合征)的一部分。CNS-HBs与嗜铬细胞瘤/副神经节瘤(PPGLs)和肾细胞癌(RCCs)在分子层面有一些相似之处。最近发现,缺氧诱导因子,尤其是体细胞HIF2A突变,在PPGLs的发病机制中起重要作用。在与红细胞增多症相关的PPGLs中已报道存在HIF2A的体细胞突变,据报道在RCCs和HBs患者中也存在。然而,目前尚不清楚CNS-HBs是否与HIF2A突变有关。我们分析了28例散发性CNS-HBs中的体细胞HIF2A和VHL突变。我们还研究了HIF靶蛋白和缺氧相关因子(HAF)的表达。发现两例散发性CNS-HBs存在体细胞HIF2A突变。一个肿瘤有2个HIF2A错义突变,其中一个先前在PPGL中被描述过(c.1121 T>A,F374Y)。第二例患者HIF2A存在体细胞截短突变(c.1669 C>T,Q557*)并伴有VHL突变。两名患者在诊断时均无红细胞增多症。我们证明HIF2A中的新型截短突变(Q557*)影响HIF-2α脯氨酰羟化,其泛素化减少但转录活性完整,从而产生激活作用。两个CNS-HB样本均显示VEGFR2/CA9/Glut1和HAF呈阳性表达。我们的数据支持VHL/HIF-2α信号通路在CNS-HBs分子发病机制中的独特核心作用,并首次显示散发性HB中存在HIF2A突变。
