Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome

Christoph Engel; Aysel Ahadova; Toni T. Seppälä; Stefan Aretz; Marloes Bigirwamungu-Bargeman; Hendrik Bläker; Karolin Bucksch; Reinhard Büttner; Wouter T. de Vos tot Nederveen Cappel; Volker Endris; Elke Holinski-Feder; Stefanie Holzapfel; Robert Hüneburg; Maarten A.J.M. Jacobs; Jan J. Koornstra; Alexandra M. Langers; Anna Lepistö; Monika Morak; Gabriela Möslein; Päivi Peltomäki; Kirsi Pylvänäinen; Nils Rahner; Laura Renkonen-Sinisalo; Karsten Schulmann; Verena Steinke-Lange; Albrecht Stenzinger; Christian P. Strassburg; Paul C. van de Meeberg; Mariette van Kouwen; Monique van Leerdam; Deepak B. Vangala; Juda Vecht; Marie Louise Verhulst; Magnus von Knebel Doeberitz; Jürgen Weitz; Silke Zachariae; Markus Loeffler; Jukka Pekka Mecklin; Matthias Kloor; Hans F. Vasen; German HNPCC Consortium, the Dutch Lynch Syndrome Collaborative Group; Finnish Lynch Syndrome Registry

doi:10.1053/j.gastro.2019.12.032

Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome

Christoph Engel^*, Aysel Ahadova, Toni T. Seppälä, Stefan Aretz, Marloes Bigirwamungu-Bargeman, Hendrik Bläker, Karolin Bucksch, Reinhard Büttner, Wouter T. de Vos tot Nederveen Cappel, Volker Endris, Elke Holinski-Feder, Stefanie Holzapfel, Robert Hüneburg, Maarten A.J.M. Jacobs, Jan J. Koornstra, Alexandra M. Langers, Anna Lepistö, Monika Morak, Gabriela Möslein, Päivi PeltomäkiKirsi Pylvänäinen, Nils Rahner, Laura Renkonen-Sinisalo, Karsten Schulmann, Verena Steinke-Lange, Albrecht Stenzinger, Christian P. Strassburg, Paul C. van de Meeberg, Mariette van Kouwen, Monique van Leerdam, Deepak B. Vangala, Juda Vecht, Marie Louise Verhulst, Magnus von Knebel Doeberitz, Jürgen Weitz, Silke Zachariae, Markus Loeffler, Jukka Pekka Mecklin, Matthias Kloor, Hans F. Vasen, German HNPCC Consortium, the Dutch Lynch Syndrome Collaborative Group, Finnish Lynch Syndrome Registry

^*Corresponding author for this work

Gastroenterology and hepatology

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Background & Aims: Lynch syndrome is caused by variants in DNA mismatch repair (MMR) genes and associated with an increased risk of colorectal cancer (CRC). In patients with Lynch syndrome, CRCs can develop via different pathways. We studied associations between Lynch syndrome–associated variants in MMR genes and risks of adenoma and CRC and somatic mutations in APC and CTNNB1 in tumors in an international cohort of patients. Methods: We combined clinical and molecular data from 3 studies. We obtained clinical data from 2747 patients with Lynch syndrome associated with variants in MLH1, MSH2, or MSH6 from Germany, the Netherlands, and Finland who received at least 2 surveillance colonoscopies and were followed for a median time of 7.8 years for development of adenomas or CRC. We performed DNA sequence analyses of 48 colorectal tumors (from 16 patients with mutations in MLH1, 29 patients with mutations in MSH2, and 3 with mutations in MSH6) for somatic mutations in APC and CTNNB1. Results: Risk of advanced adenoma in 10 years was 17.8% in patients with pathogenic variants in MSH2 vs 7.7% in MLH1 (P <.001). Higher proportions of patients with pathogenic variants in MLH1 or MSH2 developed CRC in 10 years (11.3% and 11.4%) than patients with pathogenic variants in MSH6 (4.7%) (P =.001 and P =.003 for MLH1 and MSH2 vs MSH6, respectively). Somatic mutations in APC were found in 75% of tumors from patients with pathogenic variants in MSH2 vs 11% in MLH1 (P =.015). Somatic mutations in CTNNB1 were found in 50% of tumors from patients with pathogenic variants in MLH1 vs 7% in MSH2 (P =.002). None of the 3 tumors with pathogenic variants in MSH6 had a mutation in CTNNB1, but all had mutations in APC. Conclusions: In an analysis of clinical and DNA sequence data from patients with Lynch syndrome from 3 countries, we associated pathogenic variants in MMR genes with risk of adenoma and CRC, and somatic mutations in APC and CTNNB1 in colorectal tumors. If these findings are confirmed, surveillance guidelines might be adjusted based on MMR gene variants.

Original language	English
Pages (from-to)	1326-1333
Number of pages	8
Journal	Gastroenterology
Volume	158
Issue number	5
DOIs	https://doi.org/10.1053/j.gastro.2019.12.032
Publication status	Published - Apr 2020

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10.1053/j.gastro.2019.12.032

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Engel, C., Ahadova, A., Seppälä, T. T., Aretz, S., Bigirwamungu-Bargeman, M., Bläker, H., Bucksch, K., Büttner, R., de Vos tot Nederveen Cappel, W. T., Endris, V., Holinski-Feder, E., Holzapfel, S., Hüneburg, R., Jacobs, M. A. J. M., Koornstra, J. J., Langers, A. M., Lepistö, A., Morak, M., Möslein, G., ... Finnish Lynch Syndrome Registry (2020). Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome. Gastroenterology, 158(5), 1326-1333. https://doi.org/10.1053/j.gastro.2019.12.032

@article{19a6d3f96a914d08a67891d7b8485e29,

title = "Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome",

abstract = "Background & Aims: Lynch syndrome is caused by variants in DNA mismatch repair (MMR) genes and associated with an increased risk of colorectal cancer (CRC). In patients with Lynch syndrome, CRCs can develop via different pathways. We studied associations between Lynch syndrome–associated variants in MMR genes and risks of adenoma and CRC and somatic mutations in APC and CTNNB1 in tumors in an international cohort of patients. Methods: We combined clinical and molecular data from 3 studies. We obtained clinical data from 2747 patients with Lynch syndrome associated with variants in MLH1, MSH2, or MSH6 from Germany, the Netherlands, and Finland who received at least 2 surveillance colonoscopies and were followed for a median time of 7.8 years for development of adenomas or CRC. We performed DNA sequence analyses of 48 colorectal tumors (from 16 patients with mutations in MLH1, 29 patients with mutations in MSH2, and 3 with mutations in MSH6) for somatic mutations in APC and CTNNB1. Results: Risk of advanced adenoma in 10 years was 17.8% in patients with pathogenic variants in MSH2 vs 7.7% in MLH1 (P <.001). Higher proportions of patients with pathogenic variants in MLH1 or MSH2 developed CRC in 10 years (11.3% and 11.4%) than patients with pathogenic variants in MSH6 (4.7%) (P =.001 and P =.003 for MLH1 and MSH2 vs MSH6, respectively). Somatic mutations in APC were found in 75% of tumors from patients with pathogenic variants in MSH2 vs 11% in MLH1 (P =.015). Somatic mutations in CTNNB1 were found in 50% of tumors from patients with pathogenic variants in MLH1 vs 7% in MSH2 (P =.002). None of the 3 tumors with pathogenic variants in MSH6 had a mutation in CTNNB1, but all had mutations in APC. Conclusions: In an analysis of clinical and DNA sequence data from patients with Lynch syndrome from 3 countries, we associated pathogenic variants in MMR genes with risk of adenoma and CRC, and somatic mutations in APC and CTNNB1 in colorectal tumors. If these findings are confirmed, surveillance guidelines might be adjusted based on MMR gene variants.",

keywords = "Cancer Risk, Genetic Analysis, Outcome, Prognostic Factor",

author = "Christoph Engel and Aysel Ahadova and Sepp{\"a}l{\"a}, {Toni T.} and Stefan Aretz and Marloes Bigirwamungu-Bargeman and Hendrik Bl{\"a}ker and Karolin Bucksch and Reinhard B{\"u}ttner and {de Vos tot Nederveen Cappel}, {Wouter T.} and Volker Endris and Elke Holinski-Feder and Stefanie Holzapfel and Robert H{\"u}neburg and Jacobs, {Maarten A.J.M.} and Koornstra, {Jan J.} and Langers, {Alexandra M.} and Anna Lepist{\"o} and Monika Morak and Gabriela M{\"o}slein and P{\"a}ivi Peltom{\"a}ki and Kirsi Pylv{\"a}n{\"a}inen and Nils Rahner and Laura Renkonen-Sinisalo and Karsten Schulmann and Verena Steinke-Lange and Albrecht Stenzinger and Strassburg, {Christian P.} and {van de Meeberg}, {Paul C.} and {van Kouwen}, Mariette and {van Leerdam}, Monique and Vangala, {Deepak B.} and Juda Vecht and Verhulst, {Marie Louise} and {von Knebel Doeberitz}, Magnus and J{\"u}rgen Weitz and Silke Zachariae and Markus Loeffler and Mecklin, {Jukka Pekka} and Matthias Kloor and Vasen, {Hans F.} and {German HNPCC Consortium, the Dutch Lynch Syndrome Collaborative Group} and {Finnish Lynch Syndrome Registry}",

year = "2020",

month = apr,

doi = "10.1053/j.gastro.2019.12.032",

language = "English",

volume = "158",

pages = "1326--1333",

journal = "Gastroenterology",

issn = "0016-5085",

publisher = "W.B. Saunders Ltd",

number = "5",

}

Engel, C, Ahadova, A, Seppälä, TT, Aretz, S, Bigirwamungu-Bargeman, M, Bläker, H, Bucksch, K, Büttner, R, de Vos tot Nederveen Cappel, WT, Endris, V, Holinski-Feder, E, Holzapfel, S, Hüneburg, R, Jacobs, MAJM, Koornstra, JJ, Langers, AM, Lepistö, A, Morak, M, Möslein, G, Peltomäki, P, Pylvänäinen, K, Rahner, N, Renkonen-Sinisalo, L, Schulmann, K, Steinke-Lange, V, Stenzinger, A, Strassburg, CP, van de Meeberg, PC, van Kouwen, M, van Leerdam, M, Vangala, DB, Vecht, J, Verhulst, ML, von Knebel Doeberitz, M, Weitz, J, Zachariae, S, Loeffler, M, Mecklin, JP, Kloor, M, Vasen, HF, German HNPCC Consortium, the Dutch Lynch Syndrome Collaborative Group & Finnish Lynch Syndrome Registry 2020, 'Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome', Gastroenterology, vol. 158, no. 5, pp. 1326-1333. https://doi.org/10.1053/j.gastro.2019.12.032

TY - JOUR

T1 - Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome

AU - Engel, Christoph

AU - Ahadova, Aysel

AU - Seppälä, Toni T.

AU - Aretz, Stefan

AU - Bigirwamungu-Bargeman, Marloes

AU - Bläker, Hendrik

AU - Bucksch, Karolin

AU - Büttner, Reinhard

AU - de Vos tot Nederveen Cappel, Wouter T.

AU - Endris, Volker

AU - Holinski-Feder, Elke

AU - Holzapfel, Stefanie

AU - Hüneburg, Robert

AU - Jacobs, Maarten A.J.M.

AU - Koornstra, Jan J.

AU - Langers, Alexandra M.

AU - Lepistö, Anna

AU - Morak, Monika

AU - Möslein, Gabriela

AU - Peltomäki, Päivi

AU - Pylvänäinen, Kirsi

AU - Rahner, Nils

AU - Renkonen-Sinisalo, Laura

AU - Schulmann, Karsten

AU - Steinke-Lange, Verena

AU - Stenzinger, Albrecht

AU - Strassburg, Christian P.

AU - van de Meeberg, Paul C.

AU - van Kouwen, Mariette

AU - van Leerdam, Monique

AU - Vangala, Deepak B.

AU - Vecht, Juda

AU - Verhulst, Marie Louise

AU - von Knebel Doeberitz, Magnus

AU - Weitz, Jürgen

AU - Zachariae, Silke

AU - Loeffler, Markus

AU - Mecklin, Jukka Pekka

AU - Kloor, Matthias

AU - Vasen, Hans F.

AU - German HNPCC Consortium, the Dutch Lynch Syndrome Collaborative Group

AU - Finnish Lynch Syndrome Registry

PY - 2020/4

Y1 - 2020/4

N2 - Background & Aims: Lynch syndrome is caused by variants in DNA mismatch repair (MMR) genes and associated with an increased risk of colorectal cancer (CRC). In patients with Lynch syndrome, CRCs can develop via different pathways. We studied associations between Lynch syndrome–associated variants in MMR genes and risks of adenoma and CRC and somatic mutations in APC and CTNNB1 in tumors in an international cohort of patients. Methods: We combined clinical and molecular data from 3 studies. We obtained clinical data from 2747 patients with Lynch syndrome associated with variants in MLH1, MSH2, or MSH6 from Germany, the Netherlands, and Finland who received at least 2 surveillance colonoscopies and were followed for a median time of 7.8 years for development of adenomas or CRC. We performed DNA sequence analyses of 48 colorectal tumors (from 16 patients with mutations in MLH1, 29 patients with mutations in MSH2, and 3 with mutations in MSH6) for somatic mutations in APC and CTNNB1. Results: Risk of advanced adenoma in 10 years was 17.8% in patients with pathogenic variants in MSH2 vs 7.7% in MLH1 (P <.001). Higher proportions of patients with pathogenic variants in MLH1 or MSH2 developed CRC in 10 years (11.3% and 11.4%) than patients with pathogenic variants in MSH6 (4.7%) (P =.001 and P =.003 for MLH1 and MSH2 vs MSH6, respectively). Somatic mutations in APC were found in 75% of tumors from patients with pathogenic variants in MSH2 vs 11% in MLH1 (P =.015). Somatic mutations in CTNNB1 were found in 50% of tumors from patients with pathogenic variants in MLH1 vs 7% in MSH2 (P =.002). None of the 3 tumors with pathogenic variants in MSH6 had a mutation in CTNNB1, but all had mutations in APC. Conclusions: In an analysis of clinical and DNA sequence data from patients with Lynch syndrome from 3 countries, we associated pathogenic variants in MMR genes with risk of adenoma and CRC, and somatic mutations in APC and CTNNB1 in colorectal tumors. If these findings are confirmed, surveillance guidelines might be adjusted based on MMR gene variants.

AB - Background & Aims: Lynch syndrome is caused by variants in DNA mismatch repair (MMR) genes and associated with an increased risk of colorectal cancer (CRC). In patients with Lynch syndrome, CRCs can develop via different pathways. We studied associations between Lynch syndrome–associated variants in MMR genes and risks of adenoma and CRC and somatic mutations in APC and CTNNB1 in tumors in an international cohort of patients. Methods: We combined clinical and molecular data from 3 studies. We obtained clinical data from 2747 patients with Lynch syndrome associated with variants in MLH1, MSH2, or MSH6 from Germany, the Netherlands, and Finland who received at least 2 surveillance colonoscopies and were followed for a median time of 7.8 years for development of adenomas or CRC. We performed DNA sequence analyses of 48 colorectal tumors (from 16 patients with mutations in MLH1, 29 patients with mutations in MSH2, and 3 with mutations in MSH6) for somatic mutations in APC and CTNNB1. Results: Risk of advanced adenoma in 10 years was 17.8% in patients with pathogenic variants in MSH2 vs 7.7% in MLH1 (P <.001). Higher proportions of patients with pathogenic variants in MLH1 or MSH2 developed CRC in 10 years (11.3% and 11.4%) than patients with pathogenic variants in MSH6 (4.7%) (P =.001 and P =.003 for MLH1 and MSH2 vs MSH6, respectively). Somatic mutations in APC were found in 75% of tumors from patients with pathogenic variants in MSH2 vs 11% in MLH1 (P =.015). Somatic mutations in CTNNB1 were found in 50% of tumors from patients with pathogenic variants in MLH1 vs 7% in MSH2 (P =.002). None of the 3 tumors with pathogenic variants in MSH6 had a mutation in CTNNB1, but all had mutations in APC. Conclusions: In an analysis of clinical and DNA sequence data from patients with Lynch syndrome from 3 countries, we associated pathogenic variants in MMR genes with risk of adenoma and CRC, and somatic mutations in APC and CTNNB1 in colorectal tumors. If these findings are confirmed, surveillance guidelines might be adjusted based on MMR gene variants.

KW - Cancer Risk

KW - Genetic Analysis

KW - Outcome

KW - Prognostic Factor

UR - http://www.scopus.com/inward/record.url?scp=85082058870&partnerID=8YFLogxK

U2 - 10.1053/j.gastro.2019.12.032

DO - 10.1053/j.gastro.2019.12.032

M3 - Article

C2 - 31926173

AN - SCOPUS:85082058870

VL - 158

SP - 1326

EP - 1333

JO - Gastroenterology

JF - Gastroenterology

SN - 0016-5085

IS - 5

ER -

Associations of Pathogenic Variants in MLH1, MSH2, and MSH6 With Risk of Colorectal Adenomas and Tumors and With Somatic Mutations in Patients With Lynch Syndrome

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