黑斑息肉综合征患者错构瘤性息肉和癌中的分子遗传学改变。
Molecular genetic alterations in hamartomatous polyps and carcinomas of patients with Peutz-Jeghers syndrome.
作者信息
Entius M M, Keller J J, Westerman A M, van Rees B P, van Velthuysen M L, de Goeij A F, Wilson J H, Giardiello F M, Offerhaus G J
机构信息
Department of Pathology, Academic Medical Centre/University of Amsterdam, Meibergdreef 9, 1105 AZ Amsterdam, The Netherlands.
出版信息
J Clin Pathol. 2001 Feb;54(2):126-31. doi: 10.1136/jcp.54.2.126.
AIM
To investigate whether mutations in the STK11/LKB1 gene and genes implicated in the colorectal adenoma-carcinoma sequence are involved in Peutz-Jeghers syndrome (PJS) related tumorigenesis.
METHODS
Thirty nine polyps and five carcinomas from 17 patients (from 13 families) with PJS were analysed for loss of heterozygosity (LOH) at 19p13.3 (STK11/LKB1 gene locus), 5q21 (APC gene locus), 18q21-22 (Smad4 and Smad2 gene locus), and 17p13 (p53 gene locus), and evaluated for immunohistochemical staining of p53. In addition, mutational analysis of K-ras codon 12, APC, and p53 and immunohistochemistry for Smad4 expression were performed on all carcinomas.
RESULTS
LOH at 19p was seen in 15 of the 39 polyps and in all carcinomas (n = 5). Interestingly, six of the seven polyps from patients with cancer had LOH, compared with nine of the 31 polyps from the remaining patients (p = 0.01). In one polyp from a patient without a germline STK11/LKB1 mutation, no LOH at 19p or at three alternative PJS candidate loci (19q, 6p, and 6q) was found. No LOH at 5q was observed. However, mutational analysis revealed an APC mutation in four of the five carcinomas. LOH at 17p was not seen in polyps or carcinomas; immunohistochemistry showed expression of p53 in one carcinoma and focal expression in three polyps. At subsequent sequence analysis, no p53 mutation was found. One carcinoma had an activating K-ras codon 12 mutation and another carcinoma showed 18q LOH; however, no loss of Smad4 expression was seen.
CONCLUSIONS
These results provide further evidence that STK11/LKB1 acts as a tumour suppressor gene, and may be involved in the early stages of PJS tumorigenesis. Further research is needed to see whether LOH in PJS polyps could be used as a biomarker to predict cancer. Differences in molecular genetic alterations noted between the adenoma-carcinoma sequence and PJS related tumours suggest the presence of a distinct pathway of carcinogenesis.
目的
研究丝氨酸/苏氨酸蛋白激酶11/肝脏激酶B1(STK11/LKB1)基因以及与结直肠腺瘤-癌序列相关基因的突变是否参与黑斑息肉综合征(PJS)相关的肿瘤发生过程。
方法
对17例(来自13个家族)PJS患者的39枚息肉和5例癌组织进行分析,检测19p13.3(STK11/LKB1基因位点)、5q21(腺瘤性息肉病(APC)基因位点)、18q21-22(Smad4和Smad2基因位点)以及17p13(p53基因位点)的杂合性缺失(LOH)情况,并评估p53的免疫组化染色。此外,对所有癌组织进行K-ras密码子12、APC和p53的突变分析以及Smad4表达的免疫组化检测。
结果
39枚息肉中有15枚以及所有癌组织(n = 5)均检测到19p的LOH。有趣的是,患癌患者的7枚息肉中有6枚存在LOH,而其余患者的31枚息肉中有9枚存在LOH(p = 0.01)。在1例无种系STK11/LKB1突变患者的1枚息肉中,未发现19p或其他3个PJS候选位点(19q、6p和6q)的LOH。未观察到5q的LOH。然而,突变分析显示5例癌组织中有4例存在APC突变。息肉或癌组织中均未发现17p的LOH;免疫组化显示1例癌组织中有p53表达,3枚息肉中有局灶性表达。在后续的序列分析中,未发现p53突变。1例癌组织存在激活型K-ras密码子12突变,另1例癌组织显示18q的LOH;然而,未观察到Smad4表达缺失。
结论
这些结果进一步证明STK11/LKB1作为一种肿瘤抑制基因,可能参与PJS肿瘤发生的早期阶段。需要进一步研究以确定PJS息肉中的LOH是否可作为预测癌症的生物标志物。腺瘤-癌序列与PJS相关肿瘤之间分子遗传学改变的差异提示存在独特的致癌途径。
Zotero 插件