Molecular Pathologic Analysis Enhances the Diagnosis and Management of Muir-Torre Syndrome and Gives Insight Into Its Underlying Molecular Pathogenesis

Southey, Melissa C.; Young, Mary; Whitty, Jonathan; Mifsud, Sharon; Keilar, Michelle; Mead, Leeanne J.; Trute, Lynne; Aittomäki, Kristiina; McLachlan, Sue Anne; Debinski, Henry; Venter, Deon J.; Armes, Jane E.

doi:10.1097/00000478-200107000-00013

Cited by 44 publications

(15 citation statements)

References 21 publications

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“…While there appears to be no increased risk of breast cancer in hereditary nonpolyposis colorectal cancer (HNPCC) 29,30 , we and many others have reported that a proportion of breast cancers arising in carriers of MMR gene mutations in the context of HNPCC exhibit molecular pathological evidence that the MMR gene dysfunction is associated with tumorigenesis of the breast 31,32 . MSI has been detected in a wide variety of human neoplasms associated with and without a family history of cancer and represents diagnostic criteria for mismatch repair deficiency 33,34 .…”

Section: Discussionmentioning

confidence: 94%

Molecular characterization of breast cancer in young Brazilian women

Carvalho¹,

Pereira²,

Frappart³

et al. 2010

Rev. Assoc. Med. Bras.

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SummaryObjective. To evaluate the distribution of molecular subtypes of breast tumors diagnosed in young Brazilian women and to analyze the frequency of loss of heterozygocity (LOH) in BRCA1 among different molecular subtypes of early-onset breast cancer. MethOds. Samples from 72 cases of invasive breast carcinoma diagnosed in women aged between 19 and 40 years were evaluated using an immunohistochemical panel of biomarkers. Three intragenic BRCA1 locus microsatellites, D17S1322, D17S1323, and D17S855, were PCR amplified from matched normal (lymphocyte) and tumor DNAs for (LOH) analysis. Results. We found 13 cases (18%) that had an immunohistochemical profile consistent with being basal-like. Forty cases (55%) were luminal A type; 11% (8 cases) were luminal B type, 13% (9 cases) were HER2-overexpressing tumors and two cases were ER-/HER2-carcinomas lacking basal marker expression. Four of the 16 informative cases at D17S1322, one of the four informative cases at D17S855, and none of the five informative cases at D17S1323 displayed LOH (four basal-like and one Luminal A). Microsatellite instability (MSI) at D17S855 and D17S1322 was found in two cases (one a basal-like and one Luminal A). cOnclusiOn. In our study, basal-like tumor was the second most frequent molecular type among young Brazilian women and was only observed in women diagnosed under the age of 35 years. There was no significant difference of LOH at BRCA1 locus rates between basal-like breast tumors and not-basal-like breast tumors (p=0.62). LOH in BRCA1 and MSI in these breast cancers were not frequent but may indicate a small group of breast cancers with a specific molecular makeup.

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Section: Discussionmentioning

confidence: 94%

Molecular characterization of breast cancer in young Brazilian women

Carvalho¹,

Pereira²,

Frappart³

et al. 2010

Rev. Assoc. Med. Bras.

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“…MSI testing was done on invasive tumor cells microdissected from 5-Am sections of paraffin-embedded archival tumor tissue stained with 1% methyl green. DNA extracted from histologically normal cells microdissected from colonic or lymph node tissue, or DNA extracted from peripheral blood lymphocytes, was used to control the assay as described previously (1,16,19). Ten microsatellite markers were assessed: 3 dinucleotide repeats (D5S346, D17S250, and D2S123) and 7 mononucleotide repeats (BAT25, BAT26, BAT40, MYB, TGFhRII, IGFIIR, and BAX).…”

Section: Methodsmentioning

confidence: 99%

“…For the purpose of this study, the degree of instability in each tumor was scored in two ways. The first used data from all 10 markers to categorize tumors as microsatellite stable ( 10 MS-Stable), low ( 10 MSI-Low), and high ( 10 MSI-High) when 0 to 1, 2 to 5, and 6 to 10 markers, respectively, were identified as unstable (1,16 (7). Assessment of MSI was not successful for 11 (10%) tumor samples due to technical reasons related to tumor DNA quality, leaving 107 tested tumors, which included 106 colorectal, and one stomach tumor (collected from a case where the colorectal cancer could not be located at the diagnostic laboratory).…”

Section: Methodsmentioning

confidence: 99%

“…8, 15 for examples). There is also evidence from the MSI testing of extracolonic hereditary nonpolyposis colorectal cancer -related tumors that microsatellites display tissue-specific vulnerability to instability in the presence of MMR gene mutations (16,17). A five-microsatellite marker panel for the detection of MSI was recommended in a report of a meeting on MSI at the National Cancer Institute (NCI) in 1998 (7).…”

Section: Msi-high)mentioning

confidence: 99%

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Microsatellite Instability Markers for Identifying Early-Onset Colorectal Cancers Caused by Germ-Line Mutations in DNA Mismatch Repair Genes

Mead¹,

Jenkins

Young

et al. 2007

Clinical Cancer Research

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Purpose: Microsatellite instability (MSI) testing of colorectal cancer tumors is used as a screening tool to identify patients most likely to be mismatch repair (MMR) gene mutation carriers. We wanted to examine which microsatellite markers currently used to detect MSI best predict earlyonset colorectal cancer caused by germ-line mutations in MMR genes. Experimental Design: Invasive primary tumors from a population-based sample of 107 cases of colorectal cancer diagnosed before age 45 years and tested for germ-line mutations in MLH1, MSH2, MSH6, and PMS2 and MMR protein expression were screened for MSI using the National Cancer Institute panel and an expanded 10-microsatellite marker panel. MSI-High cancers and all MLH1 and MSH2 mutation carriers (100% sensitive). Bat40 and Bat25 were unstable in all tumors of MSH6 mutation carriers (100% sensitive). Bat40 was unstable in all MMR gene mutation carriers (100% sensitive). By incorporating seven mononucleotide repeats markers into the 10-marker panel, we were able to distinguish the carriers of MSH6 mutations (all scored 10 MSI-Low) from the MLH1 and MSH2 mutation carriers (all scored 10 MSI-High). Conclusions: In early-onset colorectal cancer, a microsatellite panel containing a high proportion of mononuclear repeats can distinguish between tumors caused by MLH1 and MSH2 mutations from those caused by MSH6 mutations.

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“…At the protein level, hMLH1/hMSH2 immunohistochemistry has a role in detecting MMR defects [51][52][53] , with data suggesting that the effectiveness of immunohistochemical screening of the MMR proteins would be similar to that of the more complex strateg y of microsatellite genotyping [54] . This technique can guide which gene to sequence and can help differentiating sporadic from hereditary mutations: hMSH2 loss is likely to be HNPCC, whereas hMLH1 loss could be HNPCC or sporadic CRC (MLH1 promoter methylation).…”

Section: Immunohistochemical Testing For Mmr Defectsmentioning

confidence: 99%