Yield of routine molecular analyses in colorectal cancer patients ≤70 years to detect underlying Lynch syndrome

Lier, Margot G F van; Leenen, Celine H.; Wagner, Anja; Ramsoekh, Dewkoemar; Dubbink, Hendrikus J.; Ouweland, Ans M.W. van den; Westenend, Pieter J.; Graaf, Eelco J. R. de; Wolters, L. M. M.; Vrijland, W. W.; Kuipers, Ernst J.; Leerdam, Monique E. van; Steyerberg, Ewout W.; Dinjens, Winand N.M.

doi:10.1002/path.3963

Cited by 66 publications

(55 citation statements)

References 56 publications

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“…ing had been driven by the use of clinical guidelines based on age and family history, such as the Amsterdam (Vasen et al, 1991;Vasen et al, 1999) and Bethesda criteria (Rodriguez-Bigas et al, 1997;Umar et al, 2004). However, it has been shown that up to 50% of mutation carriers do not fulfill the Amsterdam criteria and 40-45% of families fulfilling Amsterdam criteria do not have MSI on tumor testing (Pino and Chung, 2011;Syngal et al, 2000) The Bethesda guidelines incorporate tumor histopathologic features and while more sensitive, can still miss 12-28% of LS cases (Canard et al, 2012;Hampel et al, 2008;Julie et al, 2008;Moreira et al, 2012b;van Lier et al, 2012). In 2009, the 'Jerusalem criteria' recommended IHC or MSI testing be carried out on all CRC, where the patient is under the age of 70 at diagnosis (Boland and Shike, 2010).…”

Section: Age and Clinical-based Criteriamentioning

confidence: 99%

“…Lynch syndrome (formerly hereditary non-polyposis colorectal cancer [HNPCC]) is the most common heritable cancer predisposition syndrome and is characterised by an increased predisposition to certain cancers, most notably CRC (Vasen et al, 2007). Lynch syndrome tumours are caused by autosomal dominant mutations in the DNA MMR system (Bonadona et al, 2011;Jass, 2007;Kovacs et al, 2009;Lagerstedt Robinson et al, 2007;Ligtenberg et al, 2009;Lynch et al, 2009;van der Klift et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

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The current value of determining the mismatch repair status of colorectal cancer: A rationale for routine testing

Ryan

Sheahan

Creavin

et al. 2017

Critical Reviews in Oncology/Hematology

118

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Section: Age and Clinical-based Criteriamentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The current value of determining the mismatch repair status of colorectal cancer: A rationale for routine testing

Ryan

Sheahan

Creavin

et al. 2017

Critical Reviews in Oncology/Hematology

118

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“…However, 12 to 28% of Lynch syndrome patients may be missed if testing is guided by these criteria and universal testing, that is, testing of all CRC specimens has a greater sensitivity for the identification of Lynch syndrome patients compared with the Bethesda Guidelines, but also compared with other selective strategies (e.g. tumor testing of patients with CRC < 70 years of age or older patients meeting the Bethesda Guidelines) [92,93,94,95]. It is of note that even 70% of Lynch syndrome patients may be missed when the selection is based on the pathological Bethesda criteria only, that is, CRC in a patient aged less than 50 years, CRC with MSI-H phenotype in a patient aged less than 60 years, or meta-/synchronous CRC regardless of age [43].…”

Section: Microsatellite Instability Testing In the Routine Settingmentioning

confidence: 99%

Microsatellite instability in colorectal cancer: clinicopathological significance

Setaffy¹,

Langner²

2015

pjp

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Although often viewed as a single disease, colorectal cancer more accurately represents a constellation of heterogeneous subtypes that result from different combinations of genetic events and epigenetic alterations. Chromosomal instability (CIN), microsatellite instability (MSI) and CpG island methylator phenotype (CIMP) have been identified as the three major molecular characteristics, which interact with other significant mutations, such as mutations in the KRAS and BRAF genes. High-level MSI (MSI-H) is of eminent clinical importance. It is the seminal molecular feature for the identification of individuals with Lynch syndrome, but it may also occur in sporadic cancers with CIMP phenotype, which arise from serrated precursor lesions. MSI-H status is a marker of favorable prognosis and may be used for outcome prediction, that is, molecular grading. Among others, mucinous and medullary histology, signet-ring cell differentiation, and a marked anti-tumoral immune response are histological features suggesting MSI. Universal tumor testing is recommended and may be performed using immunohistochemistry (mismatch repair protein expression) or molecular analysis, as has recently been recommended by an international task force. In this review, we consider in detail the molecular pathogenesis of colorectal cancer, focusing on the diagnosis of MSI in both hereditary and sporadic tumors.

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“…Identifying patients who have LS after their first cancer diagnosis presents the opportunity for risk-reducing strategies such as increased surveillance or prophylactic surgery. Proponents have advocated a variety of alternate screening strategies, including mathematical algorithms to predict MMR gene mutation carriers based on personal and family history [22] and broader, even universal, tumor mutation testing [14,19,23,24]. However, the inconsistency between pathologists in evaluating the histopathological features of MSI tumors [25,26,27,28] highlights the limitations of these clinical strategies.…”

Section: Discussionmentioning

confidence: 99%

Lynch Syndrome Patients with Limited Family History Identified in a Laboratory Setting: A Descriptive Study

Landon¹,

Saam²,

Brown³

et al. 2015

Oncology

1,411

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Objective: Patients diagnosed with colorectal cancer before the age of 50 years are recommended for Lynch syndrome (LS) testing according to current clinical guidelines. However, many patients are not identified because of the stringent guidelines on existing diagnostic criteria. The aim of this analysis was to evaluate the ability of existing criteria to adequately ascertain patients appropriate for LS genetic testing. Method: To determine whether existing clinical diagnostic criteria underascertain individuals who would be appropriate candidates for hereditary cancer risk assessment, we stratified the detection rate of deleterious mismatch repair (MMR) mutations in 9,109 patients with a personal history of colorectal cancer who were diagnosed between the ages of 30 and 74 years with little or no family history suggestive of LS by 5-year age-at-detection intervals. Results: There was little difference in the aggregate positive mutation rate in individuals diagnosed between the ages of 50 and 59 years compared to the positive mutation rate in patients diagnosed before the age of 50 years. Conclusion: These results suggest that cancer diagnosis under the age of 50 years is an insufficiently sensitive predictor of hereditary cancer susceptibility.

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Yield of routine molecular analyses in colorectal cancer patients ≤70 years to detect underlying Lynch syndrome

Cited by 66 publications

References 56 publications

The current value of determining the mismatch repair status of colorectal cancer: A rationale for routine testing

The current value of determining the mismatch repair status of colorectal cancer: A rationale for routine testing

Microsatellite instability in colorectal cancer: clinicopathological significance

Lynch Syndrome Patients with Limited Family History Identified in a Laboratory Setting: A Descriptive Study

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