对中枢神经系统血管母细胞瘤中VHL肿瘤抑制基因双等位基因失活的重新考量。
Reconsideration of biallelic inactivation of the VHL tumour suppressor gene in hemangioblastomas of the central nervous system.
作者信息
Gläsker S, Bender B U, Apel T W, van Velthoven V, Mulligan L M, Zentner J, Neumann H P
机构信息
Department of Nephrology and Hypertension, Albert-Ludwigs-University, Medizinische Universitätsklinik, Hugstetter Strasse 55, D 79106 Freiburg, Germany.
出版信息
J Neurol Neurosurg Psychiatry. 2001 May;70(5):644-8. doi: 10.1136/jnnp.70.5.644.
OBJECTIVES
Cerebellar haemangioblastoma occurs sporadically or as a component tumour of autosomal dominant von Hippel-Lindau disease. Biallelic inactivation of the VHL tumour suppressor gene, which is located on chromosome 3p, has been shown to be involved in the pathogenesis of both tumour entities. Mechanisms of VHL inactivation are intragenic mutations, mitotic recombination events, and hypermethylation of the promoter region. The systematic and complete examination of these genetic and epigenetic phenomena in large series of von Hippel-Lindau disease related and sporadic hemangioblastomas has, thus far, not been performed.
METHODS
In the largest series to date, 29 von Hippel-Lindau disease associated and 13 sporadic haemangioblastomas were investigated for all suggested inactivating mechanisms of the VHL gene using single strand conformational polymorphism (SSCP), loss of heterozygosity (LOH), and methylation analyses. Additionally, corresponding blood samples of all patients were screened for VHL germline mutations by SSCP and Southern blotting.
RESULTS
Germline mutations were identified in 94% of patients with von Hippel-Lindau disease and their tumours and 62% of these hemangioblastomas showed LOH of chromosome 3p. Of the 13 sporadic tumours, 23% showed a single somatic mutation of the VHL gene that was not present in the germline. 3p LOH was identified in 50% of informative sporadic tumours. No von Hippel-Lindau disease related or sporadic tumour demonstrated VHL promoter hypermethylation.
CONCLUSIONS
For most von Hippel-Lindau disease related haemangioblastomas, the inactivation or loss of both alleles of the VHL gene, as predicted by the Knudson two hit theory, is required. However, in a subset of tumours including most sporadic haemangioblastomas, the genetic pathways involved in tumorigenesis have yet to be defined and may represent alterations of a different pathway or pathways.
目的
小脑成血管细胞瘤可散发性发生,或作为常染色体显性遗传性希佩尔-林道病的组成性肿瘤出现。位于3号染色体短臂上的VHL肿瘤抑制基因的双等位基因失活已被证明与这两种肿瘤实体的发病机制有关。VHL失活的机制包括基因内突变、有丝分裂重组事件以及启动子区域的高甲基化。迄今为止,尚未对大量与希佩尔-林道病相关的和散发性成血管细胞瘤中的这些遗传和表观遗传现象进行系统而全面的研究。
方法
在迄今为止最大的系列研究中,使用单链构象多态性(SSCP)、杂合性缺失(LOH)和甲基化分析,对29例与希佩尔-林道病相关的和13例散发性成血管细胞瘤进行了VHL基因所有推测的失活机制研究。此外,通过SSCP和Southern印迹法对所有患者的相应血液样本进行VHL种系突变筛查。
结果
在94%的希佩尔-林道病患者及其肿瘤中鉴定出种系突变,其中62%的这些成血管细胞瘤显示3号染色体短臂杂合性缺失。在13例散发性肿瘤中,23%显示VHL基因的单个体细胞突变,该突变不存在于种系中。在50%的可提供信息的散发性肿瘤中鉴定出3号染色体短臂杂合性缺失。未发现与希佩尔-林道病相关的或散发性肿瘤存在VHL启动子高甲基化。
结论
对于大多数与希佩尔-林道病相关的成血管细胞瘤,如克努森二次打击理论所预测的,需要VHL基因的两个等位基因失活或缺失。然而,在包括大多数散发性成血管细胞瘤在内的一部分肿瘤中,肿瘤发生所涉及的遗传途径尚未明确,可能代表不同途径或多种途径的改变。
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