Somatic aberrations of mismatch repair genes as a cause of microsatellite‐unstable cancers

Geurts-Giele, Willemina R.R.; Leenen, Celine H.; Dubbink, Hendrikus J.; Meijssen, Isabelle C.; Post, Edward P.; Sleddens, Hein F.B.M.; Kuipers, Ernst J.; Goverde, Angelique J.; Ouweland, Ans M.W. van den; Lier, Margot G F van; Steyerberg, Ewout W.; Leerdam, Monique E. van; Wagner, Anja; Dinjens, Winand N.M.

doi:10.1002/path.4419

Cited by 137 publications

(126 citation statements)

References 41 publications

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“…There is a significant group of patients (≤35%) whose tumours have an abnormal MMR status by IHC or display MSI on molecular assays, and who have a Lynch syndrome-consistent family history, but in whom genetic testing cannot find an inherited mutation in an MMR gene, and in whom sporadic MLH1 promoter hypermethylation is not demonstrable (Geurts-Giele et al, 2014). "Lynch-like syndrome" (LLS) is a recently proposed term for such cases, and it is thought that it may account for as many as 70% of tumours in which Lynch syndrome is clinically suspected, but genetic testing fails to identify a constitutional MMR gene mutation (Rodriguez-Soler et al, 2013).…”

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

“…Patients with LLS present with cancer at younger ages, similar to Lynch syndrome (53.7 years vs. 48.5 years of age), promoting the hypothesis that undiagnosed constitutional mutations (aside from constitutional mutations in MMR genes) may also be responsible for tumor phenotypes that closely resemble Lynch syndrome (Geurts-Giele et al, 2014;Haraldsdottir et al, 2014;RodriguezSoler et al, 2013). However, it is probable that some LLS patients could actually have Lynch syndrome, as some tumours may be due to constitutional mutations in DNA MMR genes that are not detectable by standard testing.…”

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

“…Indeed extended analysis by NGS has demonstrated that in some instances this is the case (Rodriguez-Soler et al, 2013). An alternative cause is somatic mutations in an allele of a DNA MMR gene coupled with loss of heterozygosity (LOH) of the other allele (Geurts-Giele et al, 2014;Mensenkamp et al, 2014). However, up to 50% of LLS CRC exhibits biallelic somatic inactivation of DNA MMR genes within the tumor (Geurts-Giele et al, 2014;Haraldsdottir et al, 2014;Kang et al, 2015;Rodriguez-Soler et al, 2013;Sourrouille et al, 2013).…”

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

“…An alternative cause is somatic mutations in an allele of a DNA MMR gene coupled with loss of heterozygosity (LOH) of the other allele (Geurts-Giele et al, 2014;Mensenkamp et al, 2014). However, up to 50% of LLS CRC exhibits biallelic somatic inactivation of DNA MMR genes within the tumor (Geurts-Giele et al, 2014;Haraldsdottir et al, 2014;Kang et al, 2015;Rodriguez-Soler et al, 2013;Sourrouille et al, 2013). It has now been demonstrated that many of these are due to constitutional mutations and epimutations in other genes, including POLD1 and POLE (Haraldsdottir et al, 2014;Palles et al, 2013), MUTYH (Castillejo et al, 2014;Syngal et al, 2015), FAN1 (Segui et al, 2015), NTHL1 (Weren et al, 2015), PIK3CA (Cohen et al, 2016), BRCA1/2, 2 PTEN, STK11 (Yurgelun et al, 2015) and other cancer susceptibility genes (SMAD4, BMPR1A, KLLN, AKT1, AXIN2, BUB1 and BUB3) (Hansen et al, 2017) with some resultant tumours sometimes acquiring two somatic mutations in the same MMR gene, and consequently dMMR and/or MSI (Frayling and Arends, 2015;Short et al, 2015).…”

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

“…For example NGS approaches has helped identify suspected LLS patients that actually have Lynch syndrome, as some tumours may be due to constitutional mutations in DNA MMR genes that are not detectable by standard testing (Rodriguez-Soler et al, 2013). NGS testing has also identified somatic mutations coupled with LOH (Geurts-Giele et al, 2014;Haraldsdottir et al, 2014;Kang et al, 2015;Rodriguez-Soler et al, 2013;Sourrouille et al, 2013) and constitutional mutations in additional genes as causes of dMMR (Adam et al, 2016;Castillejo et al, 2014;Cohen et al, 2016;Haraldsdottir et al, 2014;Palles et al, 2013;Segui et al, 2015;Syngal et al, 2015;Weren et al, 2015).…”

Section: The Role Of Next Generation Sequencing In Determining Mmr Stmentioning

confidence: 99%

See 4 more Smart Citations

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: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

Section: "Lynch-like Syndrome" and Novel Aetiologies Of Msi Colorectamentioning

confidence: 99%

Section: The Role Of Next Generation Sequencing In Determining Mmr Stmentioning

confidence: 99%

See 3 more Smart Citations

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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Patterns of germline and somatic mutations in 16 genes associated with mismatch repair function or containing tandem repeat sequences

et al. 2019

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Background:We assumed that targeted next-generation sequencing (NGS) of mismatch repair-associated genes could improve the detection of driving mutations in colorectal cancers (CRC) with microsatellite instability (MSI) and microsatellite alterations at selected tetranucleotide repeats (EMAST) and clarify the somatic mutation patterns of CRC subtypes. Material and methods: DNAs from tumors and white blood cells were obtained from 81 patients with EMAST(+)/MSI-high (MSI-H), 78 patients with EMAST(+)/ microsatellite stable (MSS), and 72 patients with EMAST(−)/MSI-H. The germline and somatic mutations were analyzed with a 16-genes NGS panel.Results: In total, 284 germline mutations were identified in 161 patients. The most common mutations were in EPCAM (24.8%), MSH6 (24.2%), MLH1 (21.7%), and AXIN2 (21.7%). Germline mutations of AXIN2, POLE, POLD1, and TGFBR2 also resulted in EMAST and MSI. EMAST(+)/MSI-H tumors had a significant higher mutation number (205.9 ± 95.2 mut/MB) than tumors that were only EMAST(+) or MSI-H (118.6 ± 64.2 and 106.2 ± 54.5 mut/MB, respectively; both P < .001). In patients with AXIN2 germline mutations, the number of pathological somatic mutations in the tumors was significantly higher than those without AXIN2 germline mutations (176.7 ± 94.2 mut/MB vs 139.6 ± 85.0 mut/MB, P = .002). Conclusion: Next-generation sequencing could enhance the detection of familial CRC. The somatic mutation burden might result from not only the affected genes in germline mutations but also through the dysfunction of downstream effectors. The AXIN2 gene might associate with hypermutation in tumors. Further in vitro experiments to confirm the causal relationship is deserved. K E Y W O R D S colorectal cancer, EMAST, MMR, MSI, mutation | 477 CHANG et Al.

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DNA mismatch repair deficiency and hereditary syndromes in Latino patients with colorectal cancer

Ricker

Hanna

Peng

et al. 2017

Cancer

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Background The landscape of hereditary syndromes and clinicopathologic characteristics among U.S. Latinos/Hispanics with colorectal cancer (CRC) remains poorly understood. Methods A total of 265 CRC patients enrolled in the Hispanic Colorectal Cancer Study were included in this study. Information regarding CRC risk factors was elicited through interviews, and treatment and survival data was abstracted from clinical charts. Tumor studies and germline genetic testing results were collected from medical records or performed using standard molecular methods. Results The mean age at diagnosis was 53.7 years (SD=10.3), and 48.3% were female. Overall, 21.2% reported a first- or second-degree relative with CRC; 3.4% met Amsterdam I/II criteria. With respect to Bethesda guidelines, 38.5% met at least one criterion. Of the 161 individuals who had immunohistochemistry (IHC) and/or microsatellite instability (MSI) testing performed, 21 (13.0%) had mismatch repair (MMR) deficient tumors. dMMR tumors were associated with female sex (61.9%), earlier age of diagnosis (50.4 ± 12.4 years), proximal location (61.9%), and first (23.8%) or second (9.5%) degree family history of CRC. Among individuals with dMMR tumors, 13 (61.9%) had a germline MMR mutation (MLH1=6, MSH2=4, MHS6=2, and PMS2=1). We identified two additional MLH1 mutation carriers by genetic testing who had not received IHC/MSI testing. In total, 5.7% of the entire cohort were confirmed cases of Lynch syndrome. Additionally, six individuals (2.3%) had a polyposis phenotype. Conclusions The proportion of dMMR tumors in Latinos (13%) is similar to estimates in non-Hispanic Whites. The majority of individuals with dMMR tumors were confirmed to have Lynch syndrome.

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Somatic aberrations of mismatch repair genes as a cause of microsatellite‐unstable cancers

Cited by 137 publications

References 41 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

Patterns of germline and somatic mutations in 16 genes associated with mismatch repair function or containing tandem repeat sequences

DNA mismatch repair deficiency and hereditary syndromes in Latino patients with colorectal cancer

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