Miyahara H, Yane K, Naitoh H, Konishi N, Kitahori Y, Matsunaga T, Hiasa Y
NARA MED UNIV,DEPT PATHOL 2,KASHIHARA,NARA 634,JAPAN.
Int J Oncol. 1997 Jul;11(1):133-7. doi: 10.3892/ijo.11.1.133.
To examine the potential role of p53 and ras gene mutations in hypopharyngeal tumorigenesis, twenty-eight primary hypopharyngeal carcinomas, obtained at biopsy or total pharyngolaryngectomy, were investigated. Exons 5 through 9 of the p53 gene and exons 1 and 2 of the H-, K-, N-ras gene were screened using a combination of immunohistochemistry and single-strand conformation polymorphism analysis of polymerase chain reaction products (PCR-SSCP). The targeted DNA sequences coding for p53 and ras were confirmed by direct DNA sequencing. Point mutations of p53 were found in 9 (32.1%) of the 28 cases, including one with a double mutation, 3 in exon 5, 1 in exon 6, 2 in exon 7 and 4 in exon 8. Positive nuclear immunostaining for p53 was evident in 14 (50.0%) lesions. Seven (25.0%) of the 28 demonstrated point mutations in the H-rns gene, and 11 (39.3%) showed positive cytoplasmic staining for I as. The 5-year survival rate was worse with than without p53 overexpression (p <0.05). The present results suggest that gene mutations, although they occur at a relatively low incidence, are involved in hypopharyngeal tumorigenesis with p53 expression being a prognostic factor.
为研究p53和ras基因突变在下咽肿瘤发生中的潜在作用,对28例通过活检或全喉咽切除术获取的原发性下咽癌进行了研究。采用免疫组织化学和聚合酶链反应产物单链构象多态性分析(PCR-SSCP)相结合的方法,对p53基因的第5至9外显子以及H-ras、K-ras、N-ras基因的第1和第2外显子进行筛选。通过直接DNA测序对编码p53和ras的靶向DNA序列进行确认。28例中有9例(32.1%)发现p53点突变,其中1例为双突变,外显子5中有3例,外显子6中有1例,外显子7中有2例,外显子8中有4例。14例(50.0%)病变中p53核免疫染色呈阳性。28例中有7例(25.0%)显示H-ras基因点突变,11例(39.3%)显示K-ras胞质染色呈阳性。p53过表达组的5年生存率低于无p53过表达组(p<0.05)。目前的结果表明,基因突变虽发生率相对较低,但参与了下咽肿瘤的发生,p53表达是一个预后因素。
