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

Mead, Leeanne J.; Jenkins, Mark A.; Young, Joanne; Royce, Simon G.; Smith, Letitia; John, David; Macrae, Finlay; Giles, Graham G.; Hopper, John L.; Southey, Melissa C.

doi:10.1158/1078-0432.ccr-06-2174

Cited by 28 publications

(21 citation statements)

References 18 publications

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“…We decided to investigate the MSI profile of this new marker that we called MT1XT20, in a larger series of colorectal cancer cases. In comparison with previously suggested mononucleotide markers such as BAT25, BAT26, NR-21, NR-22, and NR-24 [17], in our series, MT1XT20 seems to possess very high sensitivity for detecting the MSI-H phenotype in colorectal cancer, very similar to those found for BAT26, CAT25 [15], and MybT22 [28]. Moreover, MT1XT20 revealed absolute specificity because we did not find microsatellite instability in MSS nor MSI-L cases for MT1XT20, as well as for CAT25 and MybT22.…”

Section: Discussionsupporting

confidence: 85%

T[20] repeat in the 3′-untranslated region of the MT1X gene: a marker with high sensitivity and specificity to detect microsatellite instability in colorectal cancer

Morandi

Biase

Visani

et al. 2011

Int J Colorectal Dis

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Section: Discussionsupporting

confidence: 85%

T[20] repeat in the 3′-untranslated region of the MT1X gene: a marker with high sensitivity and specificity to detect microsatellite instability in colorectal cancer

Morandi

Biase

Visani

et al. 2011

Int J Colorectal Dis

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“…Therefore, our data suggest that is possible to institute a pathology-based and more sensitive and specific method for prioritising women with early-onset breast cancer for BRCA1 mutation testing, similar to that which already applies to colorectal cancer and the DNA mismatch repair genes (Boland et al , 1998; Vasen et al , 1999; Southey et al , 2005; Lenz, 2005; Mead et al , 2007). We intend to undertake an independent study to further improve our algorithms, and we encourage others to try to validate and extend this approach, especially to later-onset disease.…”

Section: Discussionsupporting

confidence: 53%

Morphological predictors of BRCA1 germline mutations in young women with breast cancer

Southey¹,

Ramus

Dowty

et al. 2011

Br J Cancer

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Background:Knowing a young woman with newly diagnosed breast cancer has a germline BRCA1 mutation informs her clinical management and that of her relatives. We sought an optimal strategy for identifying carriers using family history, breast cancer morphology and hormone receptor status data.Methods:We studied a population-based sample of 452 Australian women with invasive breast cancer diagnosed before age 40 years for whom we conducted extensive germline mutation testing (29 carried a BRCA1 mutation) and a systematic pathology review, and collected three-generational family history and tumour ER and PR status. Predictors of mutation status were identified using multiple logistic regression. Areas under receiver operator characteristic (ROC) curves were estimated using five-fold stratified cross-validation.Results:The probability of being a BRCA1 mutation carrier increased with number of selected histology features even after adjusting for family history and ER and PR status (P<0.0001). From the most parsimonious multivariate model, the odds ratio for being a carrier were: 9.7 (95% confidence interval: 2.6–47.0) for trabecular growth pattern (P=0.001); 7.8 (2.7–25.7) for mitotic index over 50 mitoses per 10 high-powered field (P=0.0003); and 2.7 (1.3–5.9) for each first-degree relative with breast cancer diagnosed before age 60 years (P=0.01).The area under the ROC curve was 0.87 (0.83–0.90).Conclusion:Pathology review, with attention to a few specific morphological features of invasive breast cancers, can identify almost all BRCA1 germline mutation carriers among women with early-onset breast cancer without taking into account family history.

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“…The presence of an MSH6 mutation can result in a MRD tumor with a low or normal MSI status. 4,20 The second patient had a 16 base pair deletion in the PMS2 gene (PMS2 c.736 -741del16ins11) which results in a truncated protein at amino acid 246. From the normal PMS2 MMR IHC result, it must be assumed that this truncated protein is stable and contains the epitope recognized by the ␣-PMS2 antibody used in the assay.…”

Section: Discussionmentioning

confidence: 99%

Preoperative Diagnosis of Lynch Syndrome With DNA Mismatch Repair Immunohistochemistry on a Diagnostic Biopsy

Warrier

Trainer

Lynch

et al. 2011

Diseases of the Colon &Amp; Rectum

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

Cited by 28 publications

References 18 publications

T[20] repeat in the 3′-untranslated region of the MT1X gene: a marker with high sensitivity and specificity to detect microsatellite instability in colorectal cancer

T[20] repeat in the 3′-untranslated region of the MT1X gene: a marker with high sensitivity and specificity to detect microsatellite instability in colorectal cancer

Morphological predictors of BRCA1 germline mutations in young women with breast cancer

Preoperative Diagnosis of Lynch Syndrome With DNA Mismatch Repair Immunohistochemistry on a Diagnostic Biopsy

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