Increased frequency of 20q gain and copy‐neutral loss of heterozygosity in mismatch repair proficient familial colorectal carcinomas

Middeldorp, Anneke; Eijk, Ronald van; Oosting, Jan; Forte, Giusi Irma; Puijenbroek, Marjo van; Nieuwenhuizen, M. van; Corver, Willem E.; Ruano, Dina; Caldés, Trinidad; Wijnen, Juul T.; Morreau, Hans; Wezel, Tom van

doi:10.1002/ijc.26093

Cited by 23 publications

(26 citation statements)

References 48 publications

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“…42 Comparative genomic hybridization studies suggest that FCCTX tumors typically harbor 6-8 copy number alterations with recurrent gains of 7p, 7q, 8q, 13q, 20p, and 20q and losses of 17p, 18p, and 18q. 62,63 Gain of the 20q region has been specifically linked to FCCTX tumors and several candidate target genes such as 'GNAS (GNAS complex locus),' 'AURKA (aurora kinase A),' 'SRC (v-src avian sarcoma (Schmidt-Ruppin A-2) viral oncogene homolog),' 'TOP1 (topoisomerase (DNA) I),' 'NELFCD (negative elongation factor complex member C/D),' 'ADRM1 (adhesion regulating molecule 1),' 'ASIP (agouti signaling protein),' 'CDH26 (cadherin 26),' and 'HNF1A (HNF1 homeobox A)' reside herein (Figure 3). 24,62,63 GNAS promotes proliferation through activation of the Wnt and ERK1/2 MAPK signaling pathways.…”

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“…62,63 Gain of the 20q region has been specifically linked to FCCTX tumors and several candidate target genes such as 'GNAS (GNAS complex locus),' 'AURKA (aurora kinase A),' 'SRC (v-src avian sarcoma (Schmidt-Ruppin A-2) viral oncogene homolog),' 'TOP1 (topoisomerase (DNA) I),' 'NELFCD (negative elongation factor complex member C/D),' 'ADRM1 (adhesion regulating molecule 1),' 'ASIP (agouti signaling protein),' 'CDH26 (cadherin 26),' and 'HNF1A (HNF1 homeobox A)' reside herein (Figure 3). 24,62,63 GNAS promotes proliferation through activation of the Wnt and ERK1/2 MAPK signaling pathways. 64 Activating missense mutations in GNAS have been demonstrated in sporadic colorectal cancer, but the GNAS c.601G4T hot spot mutation could not be identified in a study of FCCTX tumors.…”

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confidence: 99%

“…64 Activating missense mutations in GNAS have been demonstrated in sporadic colorectal cancer, but the GNAS c.601G4T hot spot mutation could not be identified in a study of FCCTX tumors. 63,65 An overexpression of the chromosome-associated gene AURKA has been correlated to aneuploidy, invasion, and progression of colorectal adenoma to carcinoma. 66 A candidate link also exists between gain of 20q and overexpression of ASIP, that could influence sensitivity to 5-fluorouracil.…”

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confidence: 99%

“…24,25 Frequent (32%) genome-wide copy neutral loss of heterozygosity and a low frequency (14%) of chromosomal losses have been demonstrated in FCCTX tumors that could indicate involvement of yet unidentified DNA repair mechanisms. 63,68 Mutations in several cancer-related genes such as 'TP53 (tumor protein p53),' 'KRAS (Kirsten rat sarcoma viral oncogene homolog),' 'BRAF (v-raf murine sarcoma viral oncogene homolog B),' APC, 'MGMT (O-6-methylguanine-DNA methyltransferase),' and 'CTNNB1 (catenin (cadherin-associated protein), b1, 88 kDa)' divide FCCTX tumors into two major groups; one-third of the tumors that are characterized by stable genotypes with few genetic changes retained membranous b-catenin expression and infrequent TP53 mutations, and two-thirds of the tumors with frequent loss of tumor suppressor gene loci such as APC, TP53, SMAD4, and DCC, somatic methylation of APC, KRAS, and MGMT, and nuclear translocation of b-catenin. 22,69 These genetic subsets have been suggested to differ in clinical presentation; genetically simple tumors predominantly develop in the proximal colon and develop at a lower (mean 54 years) age, whereas the genetically complex tumors more often develop in the distal colon and are diagnosed at a higher (mean 59 years) age.…”

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confidence: 99%

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Familial colorectal cancer type X: genetic profiles and phenotypic features

Dominguez‐Valentin

Therkildsen²,

Silva³

et al. 2015

Modern Pathology

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Heredity is a major cause of colorectal cancer, but although several rare high-risk syndromes have been linked to disease-predisposing mutations, the genetic mechanisms are undetermined in the majority of families suspected of hereditary cancer. We review the clinical presentation, histopathologic features, and the genetic and epigenetic profiles of the familial colorectal cancer type X (FCCTX) syndrome with the aim to delineate tumor characteristics that may contribute to refined diagnostics and optimized tumor prevention.

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confidence: 99%

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Familial colorectal cancer type X: genetic profiles and phenotypic features

Dominguez‐Valentin

Therkildsen²,

Silva³

et al. 2015

Modern Pathology

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“…In particular, the frequency of 20q gain is remarkably increased when compared with sporadic colorectal cancer, suggesting that the 20q gain is involved in the genetic etiology of these mismatch repair-proficient familial colorectal cancers. 104 The finding that most of these genomic aberrations were also observed in sporadic colorectal cancer further suggests that familial and sporadic colorectal cancers could share genetic predisposition to a certain extent.…”

Section: How To Interrogate the Genetics Of Familial Colorectal Cancementioning

confidence: 99%

Gene discovery in familial cancer syndromes by exome sequencing: prospects for the elucidation of familial colorectal cancer type X

Cooper

et al. 2012

Modern Pathology

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Recent advances in genotyping and sequencing technologies have provided powerful tools with which to explore the genetic basis of both Mendelian (monogenic) and sporadic (polygenic) diseases. Several hundred genomewide association studies have so far been performed to explore the genetics of various polygenic or complex diseases including those cancers with a genetic predisposition. Exome sequencing has also proven very successful in elucidating the etiology of a range of hitherto poorly understood Mendelian disorders caused by high-penetrance mutations. Despite such progress, the genetic etiology of several familial cancers, such as familial colorectal cancer type X, has remained elusive. Familial colorectal cancer type X and Lynch syndrome are similar in terms of their fulfilling certain clinical criteria, but the former group is not characterized by germline mutations in DNA mismatch-repair genes. On the other hand, the genetics of sporadic colorectal cancer have been investigated by genome-wide association studies, leading to the identification of multiple new susceptibility loci. In addition, there is increasing evidence to suggest that familial and sporadic cancers exhibit similarities in terms of their genetic etiologies. In this review, we have summarized our current knowledge of familial colorectal cancer type X, discussed current approaches to probing its genetic etiology through the application of new sequencing technologies and the recruitment of the results of colorectal cancer genome-wide association studies, and explore the challenges that remain to be overcome given the uncertainty of the current genetic model (ie, monogenic vs polygenic) of familial colorectal cancer type X.

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Molecular patterns in the evolution of serrated lesion of the colorectum

Gaiser

Meinhardt

Hirsch

et al. 2012

Intl Journal of Cancer

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Colorectal cancer (CRC) mostly develops from a variety of polyps following mainly three different molecular pathways: chromosomal instability (CIN), microsatellite instability (MSI) and CpG island methylation (CIMP). Polyps are classified histologically as conventional adenomas, hyperplastic polyps, sessile serrated adenomas/polyps (SSA/P) and traditional serrated adenomas (TSA). However, the association of these polyps with the different types of CRCs and the underlying genetic and epigenetic aberrations has yet to be resolved. In order to address this question we analyzed 140 tumors and 20 matched mucosae by array comparative genomic hybridization, by sequence analysis of the oncogenes BRAF, KRAS, PI3K3CA and by methylation arrays. MSI was tested indirectly by immunohistochemistry (IHC) and a loss of MLH1, MSH2, MSH6 or PMS2 was assigned as high microsatellite instability (MSI‐H), while low microsatellite instability (MSI‐L) was defined as MGMT IHC negativity only. CIN was detected in 78% of all MSI‐H CRCs, most commonly as a gain of chromosome 8. Methylation data analyses allowed classification of samples into four groups and detected similar methylation profiles in SSA/P and MSI‐H CRC. TSA also revealed aberrant methylation pattern, but clustered more heterogeneously and closer to microsatellite stable (MSS) CRCs. SSA/P, TSA and MSI‐H CRCs had the highest degree of promotor methylation (CIMP pathway). Chromosomal instability, in contrast to the established doctrine, is a common phenomenon in MSI CRCs, yet to a lower extent and at later stages than in MSS CRCs. Methylation analyses suggest that SSA/P are precursors for MSI‐H CRCs and follow the CIMP pathway.

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Increased frequency of 20q gain and copy‐neutral loss of heterozygosity in mismatch repair proficient familial colorectal carcinomas

Cited by 23 publications

References 48 publications

Familial colorectal cancer type X: genetic profiles and phenotypic features

Familial colorectal cancer type X: genetic profiles and phenotypic features

Gene discovery in familial cancer syndromes by exome sequencing: prospects for the elucidation of familial colorectal cancer type X

Molecular patterns in the evolution of serrated lesion of the colorectum

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