Department of Medical Biology and Genetics, Cukurova University, 01330 Balcali-Adana, Turkey.
Cancer Epidemiol. 2010 Aug;34(4):472-7. doi: 10.1016/j.canep.2010.03.018. Epub 2010 May 4.
Chromosomal aberrations and instability of gene(s) are two factors related to the genetic instability of cancer cells. A loss of the tumor-suppressor function of the genes p16 and p53 is the most common event leading to the development of human cancers. Carcinoma of the lung is the leading cause of cancer deaths in the world. Chromosomal abnormalities in lung cancer may provide a valuable clue to the identification of target loci and culminate in a successful search for the major genes. The aim of this study was to investigate (i) alterations of the p16 and p53 genes and (ii) chromosomal aberrations in patients with small cell and non-small cell lung cancer by fluorescence in situ hybridization (FISH) and cytogenetic studies. We carried out cytogenetic analysis by Giemsa-banding in 18 cases. FISH probes for the p16 and p53 genes were also used on interphase nuclei to screen the alterations in these genes in lung cancer (LC).
We observed a high frequency of losses of the p16 - in 8/18 (44%) - and p53 - in 7/18 (39%) - genes in the cases with LC. A total of 18 patients showed predominantly numerical and structural aberrations. Among these two types, structural aberrations predominated and usually consisted of deletions, breaks, and fragilities in various chromosomes. Both structural and numerical changes were observed in almost all patients. Chromosomes 3 and 1 were found to be most frequently involved in structural abnormalities, followed by chromosomes 6, 9, and 8. Autosomal aneuploidies were also observed to be the most frequent (chromosomes 22, 19, 18, 20, 9, and 17), followed by those of the X and Y chromosomes. The expression of fragile sites was also found to be significantly higher in seven chromosomal regions: 3p14, 1q21, 1q12, 6q26, 9q13, 8q22, and 8q24.
Our data confirmed that DNA damage and genomic instability may be factors contributing to the mutation profile and development of lung cancer. The patients who developed lung cancer showed a high frequency of loss of both p16 and p53, in addition to chromosomal aberrations. Tobacco could be a major carcinogenic factor in lung-cancer progression. The loss of p16 and p53, and increased incidence of autosomal aneuploidy and chromatid breaks, along with other chromosomal alterations, can contribute to the progression of the disease.
染色体畸变和基因不稳定是与癌细胞遗传不稳定性相关的两个因素。p16 和 p53 基因的肿瘤抑制功能丧失是导致人类癌症发展的最常见事件。肺癌是世界上癌症死亡的主要原因。肺癌中的染色体异常可能为鉴定靶基因提供有价值的线索,并最终成功寻找主要基因。本研究的目的是通过荧光原位杂交(FISH)和细胞遗传学研究调查小细胞和非小细胞肺癌患者的(i)p16 和 p53 基因的改变和(ii)染色体异常。我们对 18 例进行了吉姆萨带核型分析。还使用 p16 和 p53 基因的 FISH 探针对肺癌(LC)中的这些基因进行了筛选,以检测其改变。
我们观察到 LC 中 p16 基因缺失的高频率(18 例中有 8 例,占 44%)和 p53 基因缺失的高频率(18 例中有 7 例,占 39%)。共有 18 例患者表现出主要的数值和结构异常。在这两种类型中,结构异常占主导地位,通常由各种染色体的缺失、断裂和脆性组成。几乎所有患者都观察到结构和数值变化。发现染色体 3 和 1 最常发生结构异常,其次是染色体 6、9 和 8。常染色体非整倍体也被观察到是最常见的(染色体 22、19、18、20、9 和 17),其次是 X 和 Y 染色体。在七个染色体区域还发现脆性位点的表达显著升高:3p14、1q21、1q12、6q26、9q13、8q22 和 8q24。
我们的数据证实,DNA 损伤和基因组不稳定性可能是导致肺癌突变谱和发展的因素。发生肺癌的患者除了染色体异常外,还表现出 p16 和 p53 的高频缺失。烟草可能是肺癌进展的主要致癌因素。p16 和 p53 的缺失,以及常染色体非整倍体和染色单体断裂的发生率增加,以及其他染色体改变,可能有助于疾病的进展。
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