Colorectal cancer incidence in path_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report

T Seppälä; K Pylvänäinen; Evans DG; H Järvinen; L Renkonen-Sinisalo; I Bernstein; E Holinski-Feder; P Sala; A Lindblom; F Macrae; I Blanco; R Sijmons; J Jeffries; H Vasen; J Burn; S Nakken; E Hovig; Rødland EA; K Tharmaratnam; de Vos Tot Nederveen Cappel WH; J Hill; J Wijnen; M Jenkins; Maurizio Genuardi; K Green; F Lalloo; L Sunde; M Mints; L Bertario; M Pineda; M Navarro; M Morak; Frayling IM; Plazzer JP; Sampson JR; G Capella; G Möslein; Mecklin JP; P Møller; Mallorca Group

doi:10.1186/s13053-017-0078-5

Colorectal cancer incidence in path_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report

T Seppälä^*
, K Pylvänäinen
, Evans DG
, H Järvinen
, L Renkonen-Sinisalo
, I Bernstein
, E Holinski-Feder
, P Sala
, A Lindblom
, F Macrae
, I Blanco
, R Sijmons
, J Jeffries
, H Vasen
, J Burn
, S Nakken
, E Hovig
, Rødland EA
, K Tharmaratnam
, de Vos Tot Nederveen Cappel WH

J Hill, J Wijnen, M Jenkins, Maurizio Genuardi, K Green, F Lalloo, L Sunde, M Mints, L Bertario, M Pineda, M Navarro, M Morak, Frayling IM, Plazzer JP, Sampson JR, G Capella, G Möslein, Mecklin JP, P Møller, Mallorca Group

^*Corresponding author

Research output: Contribution to journal › Article

23 Citations (Scopus)

Abstract

BACKGROUND:\r\nWe have previously reported a high incidence of colorectal cancer (CRC) in carriers of pathogenic MLH1 variants (path_MLH1) despite follow-up with colonoscopy including polypectomy.\r\n\r\nMETHODS:\r\nThe cohort included Finnish carriers enrolled in 3-yearly colonoscopy (n = 505; 4625 observation years) and carriers from other countries enrolled in colonoscopy 2-yearly or more frequently (n = 439; 3299 observation years). We examined whether the longer interval between colonoscopies in Finland could explain the high incidence of CRC and whether disease expression correlated with differences in population CRC incidence.\r\n\r\nRESULTS:\r\nCumulative CRC incidences in carriers of path_MLH1 at 70-years of age were 41% for males and 36% for females in the Finnish series and 58% and 55% in the non-Finnish series, respectively (p > 0.05). Mean time from last colonoscopy to CRC was 32.7 months in the Finnish compared to 31.0 months in the non-Finnish (p > 0.05) and was therefore unaffected by the recommended colonoscopy interval. Differences in population incidence of CRC could not explain the lower point estimates for CRC in the Finnish series. Ten-year overall survival after CRC was similar for the Finnish and non-Finnish series (88% and 91%, respectively; p > 0.05).\r\n\r\nCONCLUSIONS:\r\nThe hypothesis that the high incidence of CRC in path_MLH1 carriers was caused by a higher incidence in the Finnish series was not valid. We discuss whether the results were influenced by methodological shortcomings in our study or whether the assumption that a shorter interval between colonoscopies leads to a lower CRC incidence may be wrong. This second possibility is intriguing, because it suggests the dogma that CRC in path_MLH1 carriers develops from polyps that can be detected at colonoscopy and removed to prevent CRC may be erroneous. In view of the excellent 10-year overall survival in the Finnish and non-Finnish series we remain strong advocates of current surveillance practices for those with LS pending studies that will inform new recommendations on the best surveillance interval.

Original language	English
Pages (from-to)	18-28
Number of pages	11
Journal	Hereditary Cancer in Clinical Practice
Issue number	10
DOIs	https://doi.org/10.1186/s13053-017-0078-5
Publication status	Published - 2017

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

All Science Journal Classification (ASJC) codes

Oncology
Genetics(clinical)

Keywords

Colorectal cancer

Access to Document

10.1186/s13053-017-0078-5

Cite this

Seppälä, T., Pylvänäinen, K., DG, E., Järvinen, H., Renkonen-Sinisalo, L., Bernstein, I., Holinski-Feder, E., Sala, P., Lindblom, A., Macrae, F., Blanco, I., Sijmons, R., Jeffries, J., Vasen, H., Burn, J., Nakken, S., Hovig, E., EA, R., Tharmaratnam, K., ... Group, M. (2017). Colorectal cancer incidence in path_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report. Hereditary Cancer in Clinical Practice, (10), 18-28. https://doi.org/10.1186/s13053-017-0078-5

@article{32d8ff8823c64dacac518aeabf1acb91,

title = "Colorectal cancer incidence in path\_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report",

abstract = "BACKGROUND:\textbackslash{}r\textbackslash{}nWe have previously reported a high incidence of colorectal cancer (CRC) in carriers of pathogenic MLH1 variants (path\_MLH1) despite follow-up with colonoscopy including polypectomy.\textbackslash{}r\textbackslash{}n\textbackslash{}r\textbackslash{}nMETHODS:\textbackslash{}r\textbackslash{}nThe cohort included Finnish carriers enrolled in 3-yearly colonoscopy (n = 505; 4625 observation years) and carriers from other countries enrolled in colonoscopy 2-yearly or more frequently (n = 439; 3299 observation years). We examined whether the longer interval between colonoscopies in Finland could explain the high incidence of CRC and whether disease expression correlated with differences in population CRC incidence.\textbackslash{}r\textbackslash{}n\textbackslash{}r\textbackslash{}nRESULTS:\textbackslash{}r\textbackslash{}nCumulative CRC incidences in carriers of path\_MLH1 at 70-years of age were 41\% for males and 36\% for females in the Finnish series and 58\% and 55\% in the non-Finnish series, respectively (p > 0.05). Mean time from last colonoscopy to CRC was 32.7 months in the Finnish compared to 31.0 months in the non-Finnish (p > 0.05) and was therefore unaffected by the recommended colonoscopy interval. Differences in population incidence of CRC could not explain the lower point estimates for CRC in the Finnish series. Ten-year overall survival after CRC was similar for the Finnish and non-Finnish series (88\% and 91\%, respectively; p > 0.05).\textbackslash{}r\textbackslash{}n\textbackslash{}r\textbackslash{}nCONCLUSIONS:\textbackslash{}r\textbackslash{}nThe hypothesis that the high incidence of CRC in path\_MLH1 carriers was caused by a higher incidence in the Finnish series was not valid. We discuss whether the results were influenced by methodological shortcomings in our study or whether the assumption that a shorter interval between colonoscopies leads to a lower CRC incidence may be wrong. This second possibility is intriguing, because it suggests the dogma that CRC in path\_MLH1 carriers develops from polyps that can be detected at colonoscopy and removed to prevent CRC may be erroneous. In view of the excellent 10-year overall survival in the Finnish and non-Finnish series we remain strong advocates of current surveillance practices for those with LS pending studies that will inform new recommendations on the best surveillance interval.",

keywords = "Colorectal cancer, Colorectal cancer",

author = "T Sepp{\"a}l{\"a} and K Pylv{\"a}n{\"a}inen and Evans DG and H J{\"a}rvinen and L Renkonen-Sinisalo and I Bernstein and E Holinski-Feder and P Sala and A Lindblom and F Macrae and I Blanco and R Sijmons and J Jeffries and H Vasen and J Burn and S Nakken and E Hovig and R{\o}dland EA and K Tharmaratnam and WH, \{de Vos Tot Nederveen Cappel\} and J Hill and J Wijnen and M Jenkins and Maurizio Genuardi and K Green and F Lalloo and L Sunde and M Mints and L Bertario and M Pineda and M Navarro and M Morak and Frayling IM and Plazzer JP and Sampson JR and G Capella and G M{\"o}slein and Mecklin JP and P M{\o}ller and Mallorca Group",

year = "2017",

doi = "10.1186/s13053-017-0078-5",

language = "English",

pages = "18--28",

journal = "Hereditary Cancer in Clinical Practice",

issn = "1897-4287",

publisher = "BioMed Central",

number = "10",

}

Seppälä, T, Pylvänäinen, K, DG, E, Järvinen, H, Renkonen-Sinisalo, L, Bernstein, I, Holinski-Feder, E, Sala, P, Lindblom, A, Macrae, F, Blanco, I, Sijmons, R, Jeffries, J, Vasen, H, Burn, J, Nakken, S, Hovig, E, EA, R, Tharmaratnam, K, WH, DVTNC, Hill, J, Wijnen, J, Jenkins, M, Genuardi, M, Green, K, Lalloo, F, Sunde, L, Mints, M, Bertario, L, Pineda, M, Navarro, M, Morak, M, IM, F, JP, P, JR, S, Capella, G, Möslein, G, JP, M, Møller, P & Group, M 2017, 'Colorectal cancer incidence in path_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report', Hereditary Cancer in Clinical Practice, no. 10, pp. 18-28. https://doi.org/10.1186/s13053-017-0078-5

TY - JOUR

T1 - Colorectal cancer incidence in path_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report

AU - Seppälä, T

AU - Pylvänäinen, K

AU - DG, Evans

AU - Järvinen, H

AU - Renkonen-Sinisalo, L

AU - Bernstein, I

AU - Holinski-Feder, E

AU - Sala, P

AU - Lindblom, A

AU - Macrae, F

AU - Blanco, I

AU - Sijmons, R

AU - Jeffries, J

AU - Vasen, H

AU - Burn, J

AU - Nakken, S

AU - Hovig, E

AU - EA, Rødland

AU - Tharmaratnam, K

AU - WH, de Vos Tot Nederveen Cappel

AU - Hill, J

AU - Wijnen, J

AU - Jenkins, M

AU - Genuardi, Maurizio

AU - Green, K

AU - Lalloo, F

AU - Sunde, L

AU - Mints, M

AU - Bertario, L

AU - Pineda, M

AU - Navarro, M

AU - Morak, M

AU - IM, Frayling

AU - JP, Plazzer

AU - JR, Sampson

AU - Capella, G

AU - Möslein, G

AU - JP, Mecklin

AU - Møller, P

AU - Group, Mallorca

PY - 2017

Y1 - 2017

N2 - BACKGROUND:\r\nWe have previously reported a high incidence of colorectal cancer (CRC) in carriers of pathogenic MLH1 variants (path_MLH1) despite follow-up with colonoscopy including polypectomy.\r\n\r\nMETHODS:\r\nThe cohort included Finnish carriers enrolled in 3-yearly colonoscopy (n = 505; 4625 observation years) and carriers from other countries enrolled in colonoscopy 2-yearly or more frequently (n = 439; 3299 observation years). We examined whether the longer interval between colonoscopies in Finland could explain the high incidence of CRC and whether disease expression correlated with differences in population CRC incidence.\r\n\r\nRESULTS:\r\nCumulative CRC incidences in carriers of path_MLH1 at 70-years of age were 41% for males and 36% for females in the Finnish series and 58% and 55% in the non-Finnish series, respectively (p > 0.05). Mean time from last colonoscopy to CRC was 32.7 months in the Finnish compared to 31.0 months in the non-Finnish (p > 0.05) and was therefore unaffected by the recommended colonoscopy interval. Differences in population incidence of CRC could not explain the lower point estimates for CRC in the Finnish series. Ten-year overall survival after CRC was similar for the Finnish and non-Finnish series (88% and 91%, respectively; p > 0.05).\r\n\r\nCONCLUSIONS:\r\nThe hypothesis that the high incidence of CRC in path_MLH1 carriers was caused by a higher incidence in the Finnish series was not valid. We discuss whether the results were influenced by methodological shortcomings in our study or whether the assumption that a shorter interval between colonoscopies leads to a lower CRC incidence may be wrong. This second possibility is intriguing, because it suggests the dogma that CRC in path_MLH1 carriers develops from polyps that can be detected at colonoscopy and removed to prevent CRC may be erroneous. In view of the excellent 10-year overall survival in the Finnish and non-Finnish series we remain strong advocates of current surveillance practices for those with LS pending studies that will inform new recommendations on the best surveillance interval.

AB - BACKGROUND:\r\nWe have previously reported a high incidence of colorectal cancer (CRC) in carriers of pathogenic MLH1 variants (path_MLH1) despite follow-up with colonoscopy including polypectomy.\r\n\r\nMETHODS:\r\nThe cohort included Finnish carriers enrolled in 3-yearly colonoscopy (n = 505; 4625 observation years) and carriers from other countries enrolled in colonoscopy 2-yearly or more frequently (n = 439; 3299 observation years). We examined whether the longer interval between colonoscopies in Finland could explain the high incidence of CRC and whether disease expression correlated with differences in population CRC incidence.\r\n\r\nRESULTS:\r\nCumulative CRC incidences in carriers of path_MLH1 at 70-years of age were 41% for males and 36% for females in the Finnish series and 58% and 55% in the non-Finnish series, respectively (p > 0.05). Mean time from last colonoscopy to CRC was 32.7 months in the Finnish compared to 31.0 months in the non-Finnish (p > 0.05) and was therefore unaffected by the recommended colonoscopy interval. Differences in population incidence of CRC could not explain the lower point estimates for CRC in the Finnish series. Ten-year overall survival after CRC was similar for the Finnish and non-Finnish series (88% and 91%, respectively; p > 0.05).\r\n\r\nCONCLUSIONS:\r\nThe hypothesis that the high incidence of CRC in path_MLH1 carriers was caused by a higher incidence in the Finnish series was not valid. We discuss whether the results were influenced by methodological shortcomings in our study or whether the assumption that a shorter interval between colonoscopies leads to a lower CRC incidence may be wrong. This second possibility is intriguing, because it suggests the dogma that CRC in path_MLH1 carriers develops from polyps that can be detected at colonoscopy and removed to prevent CRC may be erroneous. In view of the excellent 10-year overall survival in the Finnish and non-Finnish series we remain strong advocates of current surveillance practices for those with LS pending studies that will inform new recommendations on the best surveillance interval.

KW - Colorectal cancer

UR - https://publicatt.unicatt.it/handle/10807/111708

UR - https://www.scopus.com/inward/citedby.uri?partnerID=HzOxMe3b&scp=85030831455&origin=inward

UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85030831455&origin=inward

U2 - 10.1186/s13053-017-0078-5

DO - 10.1186/s13053-017-0078-5

M3 - Article

SN - 1897-4287

SP - 18

EP - 28

JO - Hereditary Cancer in Clinical Practice

JF - Hereditary Cancer in Clinical Practice

IS - 10

ER -

Colorectal cancer incidence in path_MLH1 carriers subjected to different follow-up protocols: a Prospective Lynch Syndrome Database report

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