The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry

BACKGROUND: Using immunohistochemistry (IHC) to select cases for mismatch repair (MMR) genetic testing, we failed to identify a large kindred with the deleterious PMS2 mutation c.989-1G > T. The purpose of the study was to examine the sensitivity of IHC and microsatellite instability-analysis (MS...

Descripción completa

Detalles Bibliográficos
Autores principales: Grindedal, Eli Marie, Aarset, Harald, Bjørnevoll, Inga, Røyset, Elin, Mæhle, Lovise, Stormorken, Astrid, Heramb, Cecilie, Medvik, Heidi, Møller, Pål, Sjursen, Wenche
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2014
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4005455/
https://www.ncbi.nlm.nih.gov/pubmed/24790682
http://dx.doi.org/10.1186/1897-4287-12-12
_version_ 1782314104714690560
author Grindedal, Eli Marie
Aarset, Harald
Bjørnevoll, Inga
Røyset, Elin
Mæhle, Lovise
Stormorken, Astrid
Heramb, Cecilie
Medvik, Heidi
Møller, Pål
Sjursen, Wenche
author_facet Grindedal, Eli Marie
Aarset, Harald
Bjørnevoll, Inga
Røyset, Elin
Mæhle, Lovise
Stormorken, Astrid
Heramb, Cecilie
Medvik, Heidi
Møller, Pål
Sjursen, Wenche
author_sort Grindedal, Eli Marie
collection PubMed
description BACKGROUND: Using immunohistochemistry (IHC) to select cases for mismatch repair (MMR) genetic testing, we failed to identify a large kindred with the deleterious PMS2 mutation c.989-1G > T. The purpose of the study was to examine the sensitivity of IHC and microsatellite instability-analysis (MSI) to identify carriers of the mutation, and to estimate its penetrance and expressions. METHODS: All carriers and obligate carriers of the mutation were identified. All cancer diagnoses were confirmed. IHC and MSI-analysis were performed on available tumours. Penetrances of cancers included in the Amsterdam and the Bethesda Criteria, for MSI-high tumours and MSI-high and low tumours were calculated by the Kaplan-Meier algorithm. RESULTS: Probability for co-segregation of the mutation and cancers by chance was 0.000004. Fifty-six carriers or obligate carriers were identified. There was normal staining for PMS2 in 15/18 (83.3%) of tumours included in the AMS1/AMS2/Bethesda criteria. MSI-analysis showed that 15/21 (71.4%) of tumours were MSI-high and 4/21 (19.0%) were MSI-low. Penetrance at 70 years was 30.6% for AMS1 cancers (colorectal cancers), 42.8% for AMS2 cancers, 47.2% for Bethesda cancers, 55.6% for MSI-high and MSI-low cancers and 52.2% for MSI-high cancers. CONCLUSIONS: The mutation met class 5 criteria for pathogenicity. IHC was insensitive in detecting tumours caused by the mutation. Penetrance of cancers that displayed MSI was 56% at 70 years. Besides colorectal cancers, the most frequent expressions were carcinoma of the endometrium and breast in females and stomach and prostate in males.
format Online
Article
Text
id pubmed-4005455
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-40054552014-05-01 The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry Grindedal, Eli Marie Aarset, Harald Bjørnevoll, Inga Røyset, Elin Mæhle, Lovise Stormorken, Astrid Heramb, Cecilie Medvik, Heidi Møller, Pål Sjursen, Wenche Hered Cancer Clin Pract Research BACKGROUND: Using immunohistochemistry (IHC) to select cases for mismatch repair (MMR) genetic testing, we failed to identify a large kindred with the deleterious PMS2 mutation c.989-1G > T. The purpose of the study was to examine the sensitivity of IHC and microsatellite instability-analysis (MSI) to identify carriers of the mutation, and to estimate its penetrance and expressions. METHODS: All carriers and obligate carriers of the mutation were identified. All cancer diagnoses were confirmed. IHC and MSI-analysis were performed on available tumours. Penetrances of cancers included in the Amsterdam and the Bethesda Criteria, for MSI-high tumours and MSI-high and low tumours were calculated by the Kaplan-Meier algorithm. RESULTS: Probability for co-segregation of the mutation and cancers by chance was 0.000004. Fifty-six carriers or obligate carriers were identified. There was normal staining for PMS2 in 15/18 (83.3%) of tumours included in the AMS1/AMS2/Bethesda criteria. MSI-analysis showed that 15/21 (71.4%) of tumours were MSI-high and 4/21 (19.0%) were MSI-low. Penetrance at 70 years was 30.6% for AMS1 cancers (colorectal cancers), 42.8% for AMS2 cancers, 47.2% for Bethesda cancers, 55.6% for MSI-high and MSI-low cancers and 52.2% for MSI-high cancers. CONCLUSIONS: The mutation met class 5 criteria for pathogenicity. IHC was insensitive in detecting tumours caused by the mutation. Penetrance of cancers that displayed MSI was 56% at 70 years. Besides colorectal cancers, the most frequent expressions were carcinoma of the endometrium and breast in females and stomach and prostate in males. BioMed Central 2014-04-21 /pmc/articles/PMC4005455/ /pubmed/24790682 http://dx.doi.org/10.1186/1897-4287-12-12 Text en Copyright © 2014 Grindedal et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Grindedal, Eli Marie
Aarset, Harald
Bjørnevoll, Inga
Røyset, Elin
Mæhle, Lovise
Stormorken, Astrid
Heramb, Cecilie
Medvik, Heidi
Møller, Pål
Sjursen, Wenche
The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
title The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
title_full The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
title_fullStr The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
title_full_unstemmed The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
title_short The Norwegian PMS2 founder mutation c.989-1G > T shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
title_sort norwegian pms2 founder mutation c.989-1g > t shows high penetrance of microsatellite instable cancers with normal immunohistochemistry
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4005455/
https://www.ncbi.nlm.nih.gov/pubmed/24790682
http://dx.doi.org/10.1186/1897-4287-12-12
work_keys_str_mv AT grindedalelimarie thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT aarsetharald thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT bjørnevollinga thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT røysetelin thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT mæhlelovise thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT stormorkenastrid thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT herambcecilie thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT medvikheidi thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT møllerpal thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT sjursenwenche thenorwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT grindedalelimarie norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT aarsetharald norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT bjørnevollinga norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT røysetelin norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT mæhlelovise norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT stormorkenastrid norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT herambcecilie norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT medvikheidi norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT møllerpal norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry
AT sjursenwenche norwegianpms2foundermutationc9891gtshowshighpenetranceofmicrosatelliteinstablecancerswithnormalimmunohistochemistry

Ejemplares similares