Comparative genomic hybridization analysis of sporadic neuroendocrine tumors of the digestive system

Terris, Benoı̂t; Meddeb, Mounira; Marchio, Agnès; Danglot, Gisèle; Fléjou, Jean‐François; Belghiti, Jacques; Ruszniewski, Philippe; Bernheim, Alain

doi:10.1002/(sici)1098-2264(199805)22:1<50::aid-gcc7>3.0.co;2-6

Cited by 71 publications

(76 citation statements)

References 24 publications

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“…Overrepresentations of chromosome 5 are also observed in other cancers, including adrenocortical 30 and gastrointestinal endocrine tumors. 21 Because the latter study reported frequent associations of gains of chromosome 5 and 7 and, to a lesser extent, 12, and our CGH data could demonstrate 5q gains already present in three benign insulinomas, the search for a possible oncogene on chromosome 5q in EPTs seems to be justified. Two regions on 7q were mostly involved, ie, 7q11.2-q22 and 7q31.3-q32, which may harbor putative oncogenes, eg, MET at 7q31.…”

Section: Discussionsupporting

confidence: 85%

“…2 Although approximately 50% of sporadic EPTs show allelic deletions of the MEN1 gene, the mutation rate was 2 to 3 times lower in frequency, pointing to the existence of yet another TSG more telo-meric of the MEN1 gene. 5,21,22 Consistent with this hypothesis, we found losses of 11q in 36% of EPTs, with the smallest CRI at 11q13-q22. In addition, we found losses of 11p (CRI: 11p13-p14) in 30% of cases, which is in accordance with other data 10 and might point to the Wilms' tumor gene WT1 on 11p13 as a potential candidate TSG.…”

Section: Discussionmentioning

confidence: 99%

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Genetic Differences in Endocrine Pancreatic Tumor Subtypes Detected by Comparative Genomic Hybridization

Speel¹,

Richter²,

Moch³

et al. 1999

The American Journal of Pathology

144

122

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The molecular pathogenesis as well as histogenesis of endocrine pancreatic tumors (EPTs) is not well understood , and the clinical behavior of EPTs is difficult to predict using current morphological criteria. Thus, more accurate markers of risk and better understanding of tumor initiation and progression are needed to allow a precise classification of EPTs. We have studied 44 benign and malignant EPTs by comparative genomic hybridization to correlate the overall number of genetic alterations with clinical and histopathological parameters and to identify chromosomal regions which might harbor genes involved in EPT pathogenesis and progression. Aberrations were found in 36 EPTs , and chromosomal losses (mean, 5.3) were slightly more frequent than gains (mean, 4.6). The most frequent losses involved Y (45% of male EPTs) , 6q (39%) , 11q (36%) , 3p , 3q , 11p (each 30%) , 6p (27%) , and 10q and Xq (each 25%) , whereas most common gains included 7q (43%) , 17q (41%), 5q and 14q (each 32%) , 7p , 9q , 17p , 20q (each 27%), and 12q and Xp (each 25%). A correlation was found between the total number of genetic changes per tumor and both tumor size and disease stage. In particular , losses of 3p and 6 and gains of 14q and Xq were found to be associated with metastatic disease. Furthermore , characteristic patterns of genetic changes were found in the various EPT subtypes , eg , 6q loss in malignant insulinomas , indicating that these groups might evolve along genetically different pathways. The highlighted genetic aberrations , including the newly found involvement of 6q losses and sex chromosome alterations , should stimulate the further analysis of these chromosomal regions, which may lead to the discovery of novel genes important in the tumorigenesis and evolution of EPTs. (Am J Pathol 1999, 155:1787-1794)

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Section: Discussionsupporting

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Genetic Differences in Endocrine Pancreatic Tumor Subtypes Detected by Comparative Genomic Hybridization

Speel¹,

Richter²,

Moch³

et al. 1999

The American Journal of Pathology

144

122

View full text Add to dashboard Cite

show abstract

“…Using microsatellite markers, chromosome-based comparative genomic hybridization (CGH) and single nucleotide polymorphism (SNP) analysis, recurrent copy number alterations (CNAs) have been identified. The most common CNA is loss of chromosome 18 (Terris et al 1998, Zhao et al 2000, Kytölä et al 2001, Löllgen et al 2001, Tönnies et al 2001, Stancu et al 2003, Wang et al 2005, Kim do et al 2008, Kulke et al 2008. Other recurrent CNAs include losses involving chromosomes 9, 11q and/or 16q, and gains involving chromosomes 4, 5, 7, 14 and/or 20.…”

Section: Introductionmentioning

confidence: 51%

High-resolution genomic profiling reveals gain of chromosome 14 as a predictor of poor outcome in ileal carcinoids

Andersson¹,

Swärd²,

Stenman³

et al. 2009

Endocrine-Related Cancer

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Ileal carcinoids are malignant neuroendocrine tumours of the small intestine. The aim of this study was to obtain a high-resolution genomic profile of ileal carcinoids in order to define genetic changes important for tumour initiation, progression and survival. Forty-three patients with ileal carcinoids were investigated by high-resolution array-based comparative genomic hybridization. The average number of copy number alterations (CNAs) per tumour was 7

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“…Loss of 9p, 11q, 16q, and 18 in all but three tumors used in this study has been reported in our previous study using microsatellite markers , and was similar to LOH regions determined by SNP allelotyping reported in the current study. Previous studies have reported loss of 9p, 11q, 16q, and 18, and gains of chromosomal arms 4p, 17q, 19q, and 4p in WDNTs from lung and gastrointestinal tract by microsatellite analysis and comparative genomic hybridization (Terris et al, 1998;Kytö lä et al, 2001;Lö llgen et al, 2001;Tö nnies et al, 2001;Wang et al, 2005). Chromosomal aberrations were more common in PETs using the same methodology compared to WDNTs from lung and gastrointestinal tract.…”

Section: Discussionmentioning

confidence: 90%

Allelic alterations in well‐differentiated neuroendocrine tumors (carcinoid tumors) identified by genome‐wide single nucleotide polymorphism analysis and comparison with pancreatic endocrine tumors

Kim

Nagano

Choi

et al. 2007

Genes Chromosomes & Cancer

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Well-differentiated neuroendocrine tumors (WDNT, carcinoid tumors) are uncommon indolent neoplasms. The genetic alterations of these tumors are not well characterized. We used genome-wide high-density single nucleotide polymorphism (SNP) array analysis to detect copy number alterations in 29 WDNTs, including seven lung, seven nonileal gastrointestinal, and 15 ileal tumors, and compared with allelic imbalances in 15 pancreatic endocrine tumors (PETs). Most frequent allelic imbalances in WDNTs were losses of chromosome 18 in 10 tumors (34%), chromosome 21 or 21q in six (21%), chromosome 13 or 13q in five (17%) and chromosome 16 or 16q in four (14%) tumors, and amplification of chromosome 20 or 20p in seven (24%) tumors. We also found one tumor with loss of heterozygosity of chromosomes 10 and 15 without copy number loss. These allelic imbalances were associated with primary site of tumor: loss of chromosome 18 was present exclusively in ileal WDNTs (P 5 0.001), and loss of chromosome 21 or 21q was more frequent in nonileal gastrointestinal WDNTs (P 5 0.02). The tumors with loss of chromosome 21 were larger compared to tumors without loss (P 5 0.03). Chromosomal aberrations were less common in WDNTs from lung and gastrointestinal tract compared to PETs (P 5 0.001). Our study shows that genome-wide allelotyping using SNP array is a powerful new tool for the analysis of allelic imbalances in WDNTs, and some of these alterations are tumor site-dependent and are different than in PETs. V V C 2007 Wiley-Liss, Inc.

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Comparative genomic hybridization analysis of sporadic neuroendocrine tumors of the digestive system

Cited by 71 publications

References 24 publications

Genetic Differences in Endocrine Pancreatic Tumor Subtypes Detected by Comparative Genomic Hybridization

Genetic Differences in Endocrine Pancreatic Tumor Subtypes Detected by Comparative Genomic Hybridization

High-resolution genomic profiling reveals gain of chromosome 14 as a predictor of poor outcome in ileal carcinoids

Allelic alterations in well‐differentiated neuroendocrine tumors (carcinoid tumors) identified by genome‐wide single nucleotide polymorphism analysis and comparison with pancreatic endocrine tumors

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