Variation in the risk of colorectal cancer in families with Lynch syndrome: a retrospective cohort study

International Mismatch Repair Consortium

doi:10.1016/S1470-2045(21)00189-3

Variation in the risk of colorectal cancer in families with Lynch syndrome: a retrospective cohort study

International Mismatch Repair Consortium

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

83 Citations (Scopus)

Abstract

Background: Existing clinical practice guidelines for carriers of pathogenic variants of DNA mismatch repair genes (Lynch syndrome) are based on the mean age-specific cumulative risk (penetrance) of colorectal cancer for all carriers of pathogenic variants in the same gene. We aimed to estimate the variation in the penetrance of colorectal cancer between carriers of pathogenic variants in the same gene by sex and continent of residence. Methods: In this retrospective cohort study, we sourced data from the International Mismatch Repair Consortium, which comprises 273 members from 122 research centres or clinics in 32 countries from six continents who are involved in Lynch syndrome research. Families with at least three members and at least one confirmed carrier of a pathogenic or likely pathogenic variant in a DNA mismatch repair gene (MLH1, MSH2, MSH6, or PMS2) were included. The families of probands with known de-novo pathogenic variants were excluded. Data were collected on the method of ascertainment of the family, sex, carrier status, cancer diagnoses, and ages at the time of pedigree collection and at last contact or death. We used a segregation analysis conditioned on ascertainment to estimate the mean penetrance of colorectal cancer and modelled unmeasured polygenic factors to estimate the variation in penetrance. The existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers was tested by use of a Wald p value for the null hypothesis that the polygenic SD is zero. Findings: 5585 families with Lynch syndrome from 22 countries were eligible for the analysis. Of these, there were insufficient numbers to estimate penetrance for Asia and South America, and for those with EPCAM variants. Therefore, we used data (collected between July 11, 2014, and Dec 31, 2018) from 5255 families (1829 MLH1, 2179 MSH2, 798 MSH6, and 449 PMS2), comprising 79 809 relatives, recruited in 15 countries in North America, Europe, and Australasia. There was strong evidence of the existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers (p<0·0001 for each of the three three continents). These familial risk factors resulted in a wide within-gene variation in the risk of colorectal cancer for men and women from each continent who all carried pathogenic variants in the same gene or the MSH2 c.942+3A>T variant. The variation was especially prominent for MLH1 and MSH2 variant carriers, depending on gene, sex and continent, with 7–56% of carriers having a colorectal cancer penetrance of less than 20%, 9–44% having a penetrance of more than 80%, and only 10–19% having a penetrance of 40–60%. Interpretation: Our study findings highlight the important role of risk modifiers, which could lead to personalised risk assessments for precision prevention and early detection of colorectal cancer for people with Lynch syndrome. Funding: National Health and Medical Research Council, Australia.

Original language	English
Pages (from-to)	1014-1022
Number of pages	9
Journal	Lancet Oncology
Volume	22
Issue number	7
DOIs	https://doi.org/10.1016/S1470-2045(21)00189-3
Publication status	Published - Jul 2021
Externally published	Yes

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10.1016/S1470-2045(21)00189-3

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@article{77a2e29b567c44f183bfea1bb597ab28,

title = "Variation in the risk of colorectal cancer in families with Lynch syndrome: a retrospective cohort study",

abstract = "Background: Existing clinical practice guidelines for carriers of pathogenic variants of DNA mismatch repair genes (Lynch syndrome) are based on the mean age-specific cumulative risk (penetrance) of colorectal cancer for all carriers of pathogenic variants in the same gene. We aimed to estimate the variation in the penetrance of colorectal cancer between carriers of pathogenic variants in the same gene by sex and continent of residence. Methods: In this retrospective cohort study, we sourced data from the International Mismatch Repair Consortium, which comprises 273 members from 122 research centres or clinics in 32 countries from six continents who are involved in Lynch syndrome research. Families with at least three members and at least one confirmed carrier of a pathogenic or likely pathogenic variant in a DNA mismatch repair gene (MLH1, MSH2, MSH6, or PMS2) were included. The families of probands with known de-novo pathogenic variants were excluded. Data were collected on the method of ascertainment of the family, sex, carrier status, cancer diagnoses, and ages at the time of pedigree collection and at last contact or death. We used a segregation analysis conditioned on ascertainment to estimate the mean penetrance of colorectal cancer and modelled unmeasured polygenic factors to estimate the variation in penetrance. The existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers was tested by use of a Wald p value for the null hypothesis that the polygenic SD is zero. Findings: 5585 families with Lynch syndrome from 22 countries were eligible for the analysis. Of these, there were insufficient numbers to estimate penetrance for Asia and South America, and for those with EPCAM variants. Therefore, we used data (collected between July 11, 2014, and Dec 31, 2018) from 5255 families (1829 MLH1, 2179 MSH2, 798 MSH6, and 449 PMS2), comprising 79 809 relatives, recruited in 15 countries in North America, Europe, and Australasia. There was strong evidence of the existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers (p<0·0001 for each of the three three continents). These familial risk factors resulted in a wide within-gene variation in the risk of colorectal cancer for men and women from each continent who all carried pathogenic variants in the same gene or the MSH2 c.942+3A>T variant. The variation was especially prominent for MLH1 and MSH2 variant carriers, depending on gene, sex and continent, with 7–56% of carriers having a colorectal cancer penetrance of less than 20%, 9–44% having a penetrance of more than 80%, and only 10–19% having a penetrance of 40–60%. Interpretation: Our study findings highlight the important role of risk modifiers, which could lead to personalised risk assessments for precision prevention and early detection of colorectal cancer for people with Lynch syndrome. Funding: National Health and Medical Research Council, Australia.",

author = "{International Mismatch Repair Consortium} and Win, {Aung K.} and Dowty, {James G.} and Reece, {Jeanette C.} and Grant Lee and Templeton, {Allyson S.} and John-Paul Plazzer and Buchanan, {Daniel D.} and Kiwamu Akagi and Secil Aksoy and Angel Alonso and Karin Alvarez and Amor, {David J.} and Ravindran Ankathil and Stefan Aretz and Arnold, {Julie L.} and Melyssa Aronson and Rachel Austin and Ann-Sofie Backman and {Bajwa-ten Broeke}, {Sanne W.} and Ver{\'o}nica Barca-Tierno and Julian Barwell and Inge Bernstein and Pascaline Berthet and Beate Betz and Yves-Jean Bignon and Talya Boisjoli and Val{\'e}rie Bonadona and Laurent Briollais and Joan Brunet and Karolin Bucksch and Bruno Buecher and Reinhard Buettner and John Burn and Trinidad Cald{\'e}s and Gabriel Capella and Olivier Caron and Graham Casey and Chew, {Min H.} and Yun-Hee Choi and James Church and Mark Clendenning and Chrystelle Colas and Cops, {Elisa J.} and Isabelle Coupier and Marcia Cruz-Correa and {de la Chapelle}, Albert and {de Wind}, Niels and Tadeusz D{\c e}bniak and {Della Valle}, Adriana and Capuccine Delnatte and Marion Dhooge and Mev Dominguez-Valentin and Youenn Drouet and Duijkers, {Floor A.} and Chrisoph Engel and Patricia Esperon and Evans, {D. Gareth} and {Falc{\'o}n de Vargas}, A{\'i}da and Figueiredo, {Jane C.} and William Foulkes and Emmanuelle Fourme and Thierry Frebourg and Steven Gallinger and Pilar Garre and Maurizio Genuardi and Anne-Marie Gerdes and Gima, {Lauren M.} and Sophie Giraud and Annabel Goodwin and Heike G{\"o}rgens and Kate Green and Jose Guillem and Roselyne Guimbaud and Carmen Guill{\'e}n-Ponce and Guindalini, {Rodrigo S. C.} and Half, {Elizabeth E.} and Hall, {Michael J.} and Heather Hampel and Hansen, {Thomas V. O.} and Karl Heinimann and Hes, {Frederik J.} and James Hill and Ho, {Judy W. C.} and Elke Holinski-Feder and Nicoline Hoogerbrugge and Robert H{\"u}neburg and Vanessa Huntley and James, {Paul A.} and Jensen, {Uffe B.} and Thomas John and Juhari, {Wan K. W.} and Matthew Kalady and Fay Kastrinos and Matthias Kloor and Kohonen-Corish, {Maija R. J.} and Krogh, {Lotte N.} and Kupfer, {Sonia S.} and Uri Ladabaum and Kristina Lagerstedt-Robinson and Fiona Lalloo and Christine Lasset and Andrew Latchford and Pierre Laurent-Puig and Lautrup, {Charlotte K.} and Leggett, {Barbara A.} and Sophie Lejeune and Loic LeMarchand and Marjolijn Ligtenberg and Noralane Lindor and Markus Loeffler and Michel Longy and Francisco Lopez and Jan Lowery and Jan Lubi{\'n}ski and Lucassen, {Anneke M.} and Lynch, {Patrick M.} and Karolina Mali{\'n}ska and Nagahide Matsubara and Jukka-Pekka Mecklin and P{\aa}l M{\o}ller and Kevin Monahan and Morrison, {Patrick J.} and Jacob Nattermann and Matilde Navarro and Florencia Neffa and Deborah Neklason and Newcomb, {Polly A.} and Joanne Ngeow and Cassandra Nichols and Maartje Nielsen and Nixon, {Dawn M.} and Catherine Nogues and Henrik Okkels and Sylviane Olschwang and Nicholas Pachter and Pai, {Rish K.} and Palmero, {Edenir I.} and Mala Pande and Susan Parry and Patel, {Swati G.} and Rachel Pearlman and Claudia Perne and Marta Pineda and Poplawski, {Nicola K.} and Kirsi Pylv{\"a}n{\"a}inen and Jay Qiu and Nils Rahner and Raj Ramesar and Rasmussen, {Lene J.} and Silke Redler and Reis, {Rui M.} and Luigi Ricciardiello and Emilia Rogo{\.z}a-Janiszewska and Christophe Rosty and Samadder, {N. Jewel} and Sampson, {Julian R.} and Schackert, {Hans K.} and Wolff Schmiegel and Karsten Schulmann and Hel{\`e}ne Schuster and Rodney Scott and Leigha Senter and Sepp{\"a}l{\"a}, {Toni T.} and Rakefet Shtoyerman and Sijmons, {Rolf H.} and Carrie Snyder and Solomon, {Ilana B.} and Soto, {Jose Luis} and Southey, {Melissa C.} and Allan Spigelman and Florencia Spirandelli and Spurdle, {Amanda B.} and Verena Steinke-Lange and Stoffel, {Elena M.} and Strassburg, {Christian P.} and Lone Sunde and Rachel Susman and Sapna Syngal and Kohji Tanakaya and G{\"u}l{\c c}in Tezcan and Christina Therkildsen and Steve Thibodeau and Naohiro Tomita and Tucker, {Katherine M.} and Berrin Tunca and Daniela Turchetti and Nancy Uhrhammer and Joji Utsunomiya and Carlos Vaccaro and {van Duijnhoven}, {Fr{\"a}nzel J. B.} and {van Wanzeele}, {Meghan J.} and Vangala, {Deepak B.} and Vasen, {Hans F. A.} and {von Knebel Doeberitz}, Magnus and {von Salom{\'e}}, Jenny and Wadt, {Karin A. W.} and Ward, {Robyn L.} and J{\"u}rgen Weitz and Weitzel, {Jeffrey N.} and Heinric Williams and Ingrid Winship and Wise, {Paul E.} and Julie Wods and Woods, {Michael O.} and Tatsuro Yamaguchi and Silke Zachariae and Zahary, {Mohd N.} and Hopper, {John L.} and Haile, {Robert W.} and Macrae, {Finlay A.} and Gabriela M{\"o}slein and Jenkins, {Mark A.}",

year = "2021",

month = jul,

doi = "10.1016/S1470-2045(21)00189-3",

language = "English",

volume = "22",

pages = "1014--1022",

journal = "Lancet Oncology",

issn = "1470-2045",

publisher = "Lancet Publishing Group",

number = "7",

}

TY - JOUR

T1 - Variation in the risk of colorectal cancer in families with Lynch syndrome

T2 - a retrospective cohort study

AU - International Mismatch Repair Consortium

AU - Win, Aung K.

AU - Dowty, James G.

AU - Reece, Jeanette C.

AU - Lee, Grant

AU - Templeton, Allyson S.

AU - Plazzer, John-Paul

AU - Buchanan, Daniel D.

AU - Akagi, Kiwamu

AU - Aksoy, Secil

AU - Alonso, Angel

AU - Alvarez, Karin

AU - Amor, David J.

AU - Ankathil, Ravindran

AU - Aretz, Stefan

AU - Arnold, Julie L.

AU - Aronson, Melyssa

AU - Austin, Rachel

AU - Backman, Ann-Sofie

AU - Bajwa-ten Broeke, Sanne W.

AU - Barca-Tierno, Verónica

AU - Barwell, Julian

AU - Bernstein, Inge

AU - Berthet, Pascaline

AU - Betz, Beate

AU - Bignon, Yves-Jean

AU - Boisjoli, Talya

AU - Bonadona, Valérie

AU - Briollais, Laurent

AU - Brunet, Joan

AU - Bucksch, Karolin

AU - Buecher, Bruno

AU - Buettner, Reinhard

AU - Burn, John

AU - Caldés, Trinidad

AU - Capella, Gabriel

AU - Caron, Olivier

AU - Casey, Graham

AU - Chew, Min H.

AU - Choi, Yun-Hee

AU - Church, James

AU - Clendenning, Mark

AU - Colas, Chrystelle

AU - Cops, Elisa J.

AU - Coupier, Isabelle

AU - Cruz-Correa, Marcia

AU - de la Chapelle, Albert

AU - de Wind, Niels

AU - Dębniak, Tadeusz

AU - Della Valle, Adriana

AU - Delnatte, Capuccine

AU - Dhooge, Marion

AU - Dominguez-Valentin, Mev

AU - Drouet, Youenn

AU - Duijkers, Floor A.

AU - Engel, Chrisoph

AU - Esperon, Patricia

AU - Evans, D. Gareth

AU - Falcón de Vargas, Aída

AU - Figueiredo, Jane C.

AU - Foulkes, William

AU - Fourme, Emmanuelle

AU - Frebourg, Thierry

AU - Gallinger, Steven

AU - Garre, Pilar

AU - Genuardi, Maurizio

AU - Gerdes, Anne-Marie

AU - Gima, Lauren M.

AU - Giraud, Sophie

AU - Goodwin, Annabel

AU - Görgens, Heike

AU - Green, Kate

AU - Guillem, Jose

AU - Guimbaud, Roselyne

AU - Guillén-Ponce, Carmen

AU - Guindalini, Rodrigo S. C.

AU - Half, Elizabeth E.

AU - Hall, Michael J.

AU - Hampel, Heather

AU - Hansen, Thomas V. O.

AU - Heinimann, Karl

AU - Hes, Frederik J.

AU - Hill, James

AU - Ho, Judy W. C.

AU - Holinski-Feder, Elke

AU - Hoogerbrugge, Nicoline

AU - Hüneburg, Robert

AU - Huntley, Vanessa

AU - James, Paul A.

AU - Jensen, Uffe B.

AU - John, Thomas

AU - Juhari, Wan K. W.

AU - Kalady, Matthew

AU - Kastrinos, Fay

AU - Kloor, Matthias

AU - Kohonen-Corish, Maija R. J.

AU - Krogh, Lotte N.

AU - Kupfer, Sonia S.

AU - Ladabaum, Uri

AU - Lagerstedt-Robinson, Kristina

AU - Lalloo, Fiona

AU - Lasset, Christine

AU - Latchford, Andrew

AU - Laurent-Puig, Pierre

AU - Lautrup, Charlotte K.

AU - Leggett, Barbara A.

AU - Lejeune, Sophie

AU - LeMarchand, Loic

AU - Ligtenberg, Marjolijn

AU - Lindor, Noralane

AU - Loeffler, Markus

AU - Longy, Michel

AU - Lopez, Francisco

AU - Lowery, Jan

AU - Lubiński, Jan

AU - Lucassen, Anneke M.

AU - Lynch, Patrick M.

AU - Malińska, Karolina

AU - Matsubara, Nagahide

AU - Mecklin, Jukka-Pekka

AU - Møller, Pål

AU - Monahan, Kevin

AU - Morrison, Patrick J.

AU - Nattermann, Jacob

AU - Navarro, Matilde

AU - Neffa, Florencia

AU - Neklason, Deborah

AU - Newcomb, Polly A.

AU - Ngeow, Joanne

AU - Nichols, Cassandra

AU - Nielsen, Maartje

AU - Nixon, Dawn M.

AU - Nogues, Catherine

AU - Okkels, Henrik

AU - Olschwang, Sylviane

AU - Pachter, Nicholas

AU - Pai, Rish K.

AU - Palmero, Edenir I.

AU - Pande, Mala

AU - Parry, Susan

AU - Patel, Swati G.

AU - Pearlman, Rachel

AU - Perne, Claudia

AU - Pineda, Marta

AU - Poplawski, Nicola K.

AU - Pylvänäinen, Kirsi

AU - Qiu, Jay

AU - Rahner, Nils

AU - Ramesar, Raj

AU - Rasmussen, Lene J.

AU - Redler, Silke

AU - Reis, Rui M.

AU - Ricciardiello, Luigi

AU - Rogoża-Janiszewska, Emilia

AU - Rosty, Christophe

AU - Samadder, N. Jewel

AU - Sampson, Julian R.

AU - Schackert, Hans K.

AU - Schmiegel, Wolff

AU - Schulmann, Karsten

AU - Schuster, Helène

AU - Scott, Rodney

AU - Senter, Leigha

AU - Seppälä, Toni T.

AU - Shtoyerman, Rakefet

AU - Sijmons, Rolf H.

AU - Snyder, Carrie

AU - Solomon, Ilana B.

AU - Soto, Jose Luis

AU - Southey, Melissa C.

AU - Spigelman, Allan

AU - Spirandelli, Florencia

AU - Spurdle, Amanda B.

AU - Steinke-Lange, Verena

AU - Stoffel, Elena M.

AU - Strassburg, Christian P.

AU - Sunde, Lone

AU - Susman, Rachel

AU - Syngal, Sapna

AU - Tanakaya, Kohji

AU - Tezcan, Gülçin

AU - Therkildsen, Christina

AU - Thibodeau, Steve

AU - Tomita, Naohiro

AU - Tucker, Katherine M.

AU - Tunca, Berrin

AU - Turchetti, Daniela

AU - Uhrhammer, Nancy

AU - Utsunomiya, Joji

AU - Vaccaro, Carlos

AU - van Duijnhoven, Fränzel J. B.

AU - van Wanzeele, Meghan J.

AU - Vangala, Deepak B.

AU - Vasen, Hans F. A.

AU - von Knebel Doeberitz, Magnus

AU - von Salomé, Jenny

AU - Wadt, Karin A. W.

AU - Ward, Robyn L.

AU - Weitz, Jürgen

AU - Weitzel, Jeffrey N.

AU - Williams, Heinric

AU - Winship, Ingrid

AU - Wise, Paul E.

AU - Wods, Julie

AU - Woods, Michael O.

AU - Yamaguchi, Tatsuro

AU - Zachariae, Silke

AU - Zahary, Mohd N.

AU - Hopper, John L.

AU - Haile, Robert W.

AU - Macrae, Finlay A.

AU - Möslein, Gabriela

AU - Jenkins, Mark A.

PY - 2021/7

Y1 - 2021/7

N2 - Background: Existing clinical practice guidelines for carriers of pathogenic variants of DNA mismatch repair genes (Lynch syndrome) are based on the mean age-specific cumulative risk (penetrance) of colorectal cancer for all carriers of pathogenic variants in the same gene. We aimed to estimate the variation in the penetrance of colorectal cancer between carriers of pathogenic variants in the same gene by sex and continent of residence. Methods: In this retrospective cohort study, we sourced data from the International Mismatch Repair Consortium, which comprises 273 members from 122 research centres or clinics in 32 countries from six continents who are involved in Lynch syndrome research. Families with at least three members and at least one confirmed carrier of a pathogenic or likely pathogenic variant in a DNA mismatch repair gene (MLH1, MSH2, MSH6, or PMS2) were included. The families of probands with known de-novo pathogenic variants were excluded. Data were collected on the method of ascertainment of the family, sex, carrier status, cancer diagnoses, and ages at the time of pedigree collection and at last contact or death. We used a segregation analysis conditioned on ascertainment to estimate the mean penetrance of colorectal cancer and modelled unmeasured polygenic factors to estimate the variation in penetrance. The existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers was tested by use of a Wald p value for the null hypothesis that the polygenic SD is zero. Findings: 5585 families with Lynch syndrome from 22 countries were eligible for the analysis. Of these, there were insufficient numbers to estimate penetrance for Asia and South America, and for those with EPCAM variants. Therefore, we used data (collected between July 11, 2014, and Dec 31, 2018) from 5255 families (1829 MLH1, 2179 MSH2, 798 MSH6, and 449 PMS2), comprising 79 809 relatives, recruited in 15 countries in North America, Europe, and Australasia. There was strong evidence of the existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers (p<0·0001 for each of the three three continents). These familial risk factors resulted in a wide within-gene variation in the risk of colorectal cancer for men and women from each continent who all carried pathogenic variants in the same gene or the MSH2 c.942+3A>T variant. The variation was especially prominent for MLH1 and MSH2 variant carriers, depending on gene, sex and continent, with 7–56% of carriers having a colorectal cancer penetrance of less than 20%, 9–44% having a penetrance of more than 80%, and only 10–19% having a penetrance of 40–60%. Interpretation: Our study findings highlight the important role of risk modifiers, which could lead to personalised risk assessments for precision prevention and early detection of colorectal cancer for people with Lynch syndrome. Funding: National Health and Medical Research Council, Australia.

AB - Background: Existing clinical practice guidelines for carriers of pathogenic variants of DNA mismatch repair genes (Lynch syndrome) are based on the mean age-specific cumulative risk (penetrance) of colorectal cancer for all carriers of pathogenic variants in the same gene. We aimed to estimate the variation in the penetrance of colorectal cancer between carriers of pathogenic variants in the same gene by sex and continent of residence. Methods: In this retrospective cohort study, we sourced data from the International Mismatch Repair Consortium, which comprises 273 members from 122 research centres or clinics in 32 countries from six continents who are involved in Lynch syndrome research. Families with at least three members and at least one confirmed carrier of a pathogenic or likely pathogenic variant in a DNA mismatch repair gene (MLH1, MSH2, MSH6, or PMS2) were included. The families of probands with known de-novo pathogenic variants were excluded. Data were collected on the method of ascertainment of the family, sex, carrier status, cancer diagnoses, and ages at the time of pedigree collection and at last contact or death. We used a segregation analysis conditioned on ascertainment to estimate the mean penetrance of colorectal cancer and modelled unmeasured polygenic factors to estimate the variation in penetrance. The existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers was tested by use of a Wald p value for the null hypothesis that the polygenic SD is zero. Findings: 5585 families with Lynch syndrome from 22 countries were eligible for the analysis. Of these, there were insufficient numbers to estimate penetrance for Asia and South America, and for those with EPCAM variants. Therefore, we used data (collected between July 11, 2014, and Dec 31, 2018) from 5255 families (1829 MLH1, 2179 MSH2, 798 MSH6, and 449 PMS2), comprising 79 809 relatives, recruited in 15 countries in North America, Europe, and Australasia. There was strong evidence of the existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers (p<0·0001 for each of the three three continents). These familial risk factors resulted in a wide within-gene variation in the risk of colorectal cancer for men and women from each continent who all carried pathogenic variants in the same gene or the MSH2 c.942+3A>T variant. The variation was especially prominent for MLH1 and MSH2 variant carriers, depending on gene, sex and continent, with 7–56% of carriers having a colorectal cancer penetrance of less than 20%, 9–44% having a penetrance of more than 80%, and only 10–19% having a penetrance of 40–60%. Interpretation: Our study findings highlight the important role of risk modifiers, which could lead to personalised risk assessments for precision prevention and early detection of colorectal cancer for people with Lynch syndrome. Funding: National Health and Medical Research Council, Australia.

UR - http://www.scopus.com/inward/record.url?scp=85108809980&partnerID=8YFLogxK

U2 - 10.1016/S1470-2045(21)00189-3

DO - 10.1016/S1470-2045(21)00189-3

M3 - Article

C2 - 34111421

SN - 1470-2045

VL - 22

SP - 1014

EP - 1022

JO - Lancet Oncology

JF - Lancet Oncology

IS - 7

ER -

Variation in the risk of colorectal cancer in families with Lynch syndrome: a retrospective cohort study

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