Feng X, Zhang S, Ichikawa T, Koga H, Washiyama K, Motoyama T, Kumanishi T
Department of Neuropathology, Niigata University.
Jpn J Cancer Res. 1995 Jun;86(6):555-61. doi: 10.1111/j.1349-7006.1995.tb02434.x.
Using polymerase chain reaction-single-strand conformation polymorphism (PCR-SSCP) analysis, p53 gene mutation was examined in 12 intracranial germ cell tumors (5 yolk sac carcinomas and 7 germinomas), many of which were derived from young patients in the first to the second decade. A total of 10 mutations were detected in 4 of the 12 cases and, in 3 of them, the mutations were multiple or tandem. Among the 10 mutations, 7 were missense, 1 was splicing and 2 were silent. The 7 missense mutations were located at previously proposed hot spot codons or in their vicinity or, when outside the hot spots, at a codon encoding an amino acid conserved in most vertebrates. These findings suggested that all 7 missense mutations may actually give rise to functional alteration of the p53 protein. The splicing mutation was considered to be a germ-line mutation, though its biological effect was equivocal, since the neoplastic tissue contained an additional mutation. The pattern of the mutations was predominancy of G:C-A:T transition with frequent involvement of the CpG site. These mutations were more frequently detected in yolk sac carcinomas (60%; 3/5 cases) than in germinomas (14%; 1/7 cases), suggesting that the contribution of the p53 mutation to carcinogenesis differed with the histological type of the intracranial germ cell tumor.
采用聚合酶链反应-单链构象多态性(PCR-SSCP)分析方法,对12例颅内生殖细胞肿瘤(5例卵黄囊癌和7例生殖细胞瘤)进行了p53基因突变检测,其中许多病例来自10至20岁的年轻患者。12例中有4例共检测到10个突变,其中3例为多个或串联突变。10个突变中,7个为错义突变,1个为剪接突变,2个为沉默突变。7个错义突变位于先前提出的热点密码子或其附近,或者在热点之外时,位于编码大多数脊椎动物中保守氨基酸的密码子处。这些发现表明,所有7个错义突变实际上可能导致p53蛋白的功能改变。尽管其生物学效应不明确,但由于肿瘤组织中存在另一个突变,该剪接突变被认为是种系突变。突变模式以G:C-A:T转换为主,且频繁涉及CpG位点。这些突变在卵黄囊癌(60%;3/5例)中比在生殖细胞瘤(14%;1/7例)中更频繁地被检测到,这表明p53突变对颅内生殖细胞肿瘤致癌作用的贡献因组织学类型而异。
