Rey J A, Pestaña A, Bello M J
Instituto de Investigaciones Biomédicas (CSIC), Madrid, Spain.
Oncol Res. 1992;4(8-9):321-31.
Cytogenic and molecular genetic analyses of the major histological subtypes of nervous system tumors, gliomas, meningiomas, and neurinomas, have provided interesting information on the mechanisms responsible for or contributing to their origin and development. Regarding malignant gliomas, a complex pattern of chromosomal involvement has been documented at the cytogenetic level: gains of chromosome 7 and losses of chromosome 10, 9p, 17p, and 22; further molecular characterization of these abnormalities has shown that mutational alterations of the p53 gene, together with the loss of alleles at 17p, seem to be the earliest abnormalities occurring during the genesis and progression of these neoplasms. The losses of regions on chromosomes 22 and 13 might also be relatively early events, perhaps characterizing subgroups of low grade gliomas. The mutations of the p53 gene in low grade tumors leads to a selective advantage in vivo and seems to be a critical step in the transformation from low grade to high grade gliomas. The loss of sequences on chromosome 10 and the deletions of 9p (that is loss of tumor suppressor genes on these locations), and epidermal growth factor receptor gene amplification, have been proposed as sequential abnormalities participating in glioblastoma tumorigenesis. The available data on meningiomas and neurinomas show that loss of regions on chromosome 22 is the main characteristic feature. Thus, tumor suppressor genes located in this chromosome are non-randomly involved in both neoplasms, and may present as solitary, sporadic tumors or as multiple associated lesions in neurofibromatosis type 2 (NF-2). The molecular analysis of a large series of meningiomas to determine the common chromosome 22 region lost has revealed that a putative meningioma tumor suppressor gene should be located at the distal 22q12.3-qter region. In parallel, the linkage data on the mapping of the NF-2 gene suggest that the NF-2 and meningioma loci are separate entities. However, some evidence exists on a possible participation of the NF-2 locus in the genesis of some meningiomas. The efforts to identify and isolate the genes involved, as well as their functional analysis, will contribute to a better understanding of the mechanisms of oncogenesis in these neoplasms and will doubtless have a clinical impact in the diagnosis, treatment and prognosis of nervous system tumors in patients.
对神经系统肿瘤的主要组织学亚型,即胶质瘤、脑膜瘤和神经鞘瘤进行的细胞遗传学和分子遗传学分析,为其起源和发展的相关机制提供了有趣的信息。关于恶性胶质瘤,在细胞遗传学水平已记录到复杂的染色体受累模式:7号染色体增加以及10号、9p、17p和22号染色体缺失;对这些异常的进一步分子特征分析表明,p53基因的突变改变以及17p等位基因的缺失,似乎是这些肿瘤发生和进展过程中最早出现的异常。22号和13号染色体区域的缺失也可能是相对早期的事件,或许可作为低级别胶质瘤亚组的特征。低级别肿瘤中p53基因的突变在体内导致选择性优势,似乎是低级别胶质瘤向高级别胶质瘤转变的关键步骤。10号染色体序列缺失和9p缺失(即这些位置的肿瘤抑制基因丢失)以及表皮生长因子受体基因扩增,被认为是参与胶质母细胞瘤肿瘤发生的一系列异常。关于脑膜瘤和神经鞘瘤的现有数据表明,22号染色体区域缺失是主要特征。因此,位于该染色体上的肿瘤抑制基因非随机地参与这两种肿瘤,可能表现为散发性孤立肿瘤或作为2型神经纤维瘤病(NF - 2)中的多个相关病变。对大量脑膜瘤进行分子分析以确定22号染色体上共同缺失区域,结果显示一个假定的脑膜瘤肿瘤抑制基因应位于22q12.3 - qter远端区域。同时,NF - 2基因定位的连锁数据表明NF - 2和脑膜瘤基因座是不同的实体。然而,有一些证据表明NF - 2基因座可能参与某些脑膜瘤的发生。识别和分离相关基因以及对其进行功能分析的努力,将有助于更好地理解这些肿瘤的肿瘤发生机制,无疑会对神经系统肿瘤患者的诊断、治疗和预后产生临床影响。
