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Loss of 11p11 is a frequent and early event in sporadic nonfunctioning pancreatic neuroendocrine neoplasms

机译:11p11的丢失是偶发性非功能性胰腺神经内分泌肿瘤中的常见事件。

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摘要

The pathogenesis of sporadic pancreatic neuroendocrine neoplasms (PNENs) is poorly understood. To gain insight into the genetic mechanisms underlying this tumor entity, we performed genome-wide screening of 16 surgical specimens from 15 patients with sporadic PNEN, combining G-band karyotyping and high resolution comparative genomic hybridization (HR-CGH). G-banding revealed abnormal karyotypes in 2 of 10 tumor samples analyzed. DNA copy number changes were detected in 13 samples, whereas three tumors showed a balanced genome. Gains were more frequent than losses in the nonfunctioning tumors (n=13). Common gains were scored at 5p12–13, 4q13–24, 5p15, 5q11–31, and 9q21–22. Common losses were scored at 11p11, 11p14–15, 11q23, 11p12–13, and 11q22. The average number of copy aberrations (ANCA index) was 12 for 13 nonfunctioning primary tumors, 4.8 for the nonfunctioning tumors with low Ki-67 (≥5%), 21.2 for the tumors with high Ki-67 (<5%), 2.5 for small tumors (<3.5 cm), and 17.8 for large tumors (≥3.5 cm). There was a statistically significant difference in the ANCA index between the groups defined by Ki-67 and tumor size. Nonfunctioning tumors with low Ki-67, no distant metastasis and small size had few aberrations detected by HR-CGH, but frequent loss of material from chromosomal band 11p11. The present study indicates the existence of distinct cytogenetic patterns in sporadic nonfunctioning PNEN. Loss of chromosomal band 11p11 might indicate a primary pathogenetic event in these tumors.
机译:零星胰腺神经内分泌肿瘤(PNENs)的发病机理了解甚少。为了深入了解该肿瘤实体的遗传机制,我们结合了G波段核型和高分辨率比较基因组杂交(HR-CGH),对来自15例散发性PNEN患者的16例手术标本进行了全基因组筛选。 G谱带显示分析的10个肿瘤样本中有2个的核型异常。在13个样品中检测到DNA拷贝数变化,而三个肿瘤显示出平衡的基因组。在无功能的肿瘤中,获得比丢失更频繁(n = 13)。常见收获得分为5p12-13、4q13-24、5p15、5q11-31和9q21-22。常见损失分为11p11、11p14-15、11q23、11p12-13和11q22。平均13个非功能性原发肿瘤的平均拷贝畸变数(ANCA指数),Ki-67低(≥5%)的非功能性肿瘤的4.8,Ki-67高(<5%)的肿瘤的21.2的2.5对于小肿瘤(<3.5 cm),大肿瘤(≥3.5cm)为17.8。 Ki-67定义的各组之间的ANCA指数与肿瘤大小之间存在统计学上的显着差异。 Ki-67低,无远处转移且体积小的无功能肿瘤,HR-CGH检出的畸变极少,但从11p11染色体带中频繁丢失物质。本研究表明在散发性非功能性PNEN中存在独特的细胞遗传学模式。染色体带11p11的丢失可能表明这些肿瘤中的主要致病事件。

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