Figueiredo B C, Stratakis C A, Sandrini R, DeLacerda L, Pianovsky M A, Giatzakis C, Young H M, Haddad B R
Department of Pediatrics, Federal University of Paraná, Curitiba, Brazil.
J Clin Endocrinol Metab. 1999 Mar;84(3):1116-21. doi: 10.1210/jcem.84.3.5526.
Although several genes have been investigated in adrenal tumorigenesis, the genetic background of adrenocortical tumors (ACT) remains poorly characterized. In southern Brazil, the annual incidence of ACT is unusually high, ranging from 3.4-4.2/million children, compared with a worldwide incidence of 0.3/million children younger than 15 yr. Environmental factors have been implicated because the distribution of these tumors follows a regional, rather than a familial, pattern. However, decreased penetrance of a particular gene defect cannot be excluded. Because linkage or other traditional genetic analyses would not be appropriate to investigate the defect(s) associated with ACT in this population, we used comparative genomic hybridization (CGH) to screen for DNA sequence copy number changes in 9 nonfamilial ACT (6 carcinomas and 3 adenomas) from unrelated patients from this region. Six female (aged 10 months to 6 3/4 yr) and 3 male (1 1/12 to 3 1/4 yr) patients were studied. Three carcinomas were at stage I, 1 was at stage II, and another was at stage III. Two carcinomas had evidence of invasion of the vena cava, and 3 were more than 3 cm in size. All patients underwent surgical excision of their tumors; chemotherapy was administered to cancer patients. Currently, all patients are alive and in remission, with the exception of 1 patient with stage III cancer. High mol wt DNA was extracted from tumor tissue obtained at surgery and frozen at -70 C. This DNA was labeled and used for CGH according to standard procedures. Digital image analysis was performed to detect chromosomal gains or losses. CGH evaluation revealed extensive genetic aberrations in both adenomas and carcinomas; there were no significant differences relative to age, gender, size, or stage of the tumor (P > 0.1). Chromosomes and chromosomal regions 1q, 5p, 5q, 6p, 6q, 8p, 8q, 9q, 10p, 11q, 12q, 13q, 14q, 15q, 16, 18q, 19, and 20q demonstrated gains, whereas 2q, 3, 4, 9p, 11, 13q, 18, 20p, and Xq showed losses. The most striking finding was consistent copy number gain of chromosomal region 9q34 in 8 of the 9 tumors. We conclude that both benign and malignant ACT from southern Brazil show multiple genetic aberrations, including a consistent gain of chromosomal region 9q34. This genomic area may harbor genetic defects that predispose to ACT formation and are shared by the patients who were investigated in this study or are accumulated epigenetically under the influence of a common factor, such as an environmental mutagen.
尽管已经对几种基因在肾上腺肿瘤发生过程中的作用进行了研究,但肾上腺皮质肿瘤(ACT)的遗传背景仍未得到充分表征。在巴西南部,ACT的年发病率异常高,为每百万儿童3.4 - 4.2例,而全球15岁以下儿童的发病率为每百万0.3例。由于这些肿瘤的分布呈现区域性而非家族性模式,因此环境因素被认为与之相关。然而,不能排除特定基因缺陷的外显率降低的情况。由于连锁分析或其他传统遗传分析不适用于研究该人群中与ACT相关的缺陷,我们使用比较基因组杂交(CGH)技术,对该地区9例非家族性ACT(6例癌和3例腺瘤)患者的DNA序列拷贝数变化进行筛查。研究对象包括6名女性(年龄从10个月至6又3/4岁)和3名男性(1又1/12至3又1/4岁)患者。3例癌处于I期,1例处于II期,另1例处于III期。2例癌有腔静脉侵犯的证据,3例肿瘤大小超过3厘米。所有患者均接受了肿瘤手术切除;癌症患者接受了化疗。目前,除1例III期癌症患者外,所有患者均存活且处于缓解期。从手术中获取的肿瘤组织中提取高分子量DNA,并在-70℃下冷冻保存。按照标准程序对该DNA进行标记并用于CGH分析。通过数字图像分析检测染色体的增加或减少。CGH评估显示腺瘤和癌中均存在广泛的基因畸变;相对于肿瘤的年龄、性别、大小或分期,差异均无统计学意义(P>0.1)。染色体及染色体区域1q、5p、5q、6p、6q、8p、8q、9q、10p、11q、12q、13q、14q、15q、16、18q、19和20q显示有增加,而2q、3、4、9p、11、13q、18、20p和Xq显示有减少。最显著的发现是9例肿瘤中的8例染色体区域9q34存在一致的拷贝数增加。我们得出结论,巴西南部的良性和恶性ACT均显示出多种基因畸变,包括染色体区域9q34的一致增加。该基因组区域可能存在导致ACT形成的基因缺陷,这些缺陷为本研究中的患者所共有,或者是在共同因素(如环境诱变剂)的影响下通过表观遗传积累产生的。
