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Double somatic mutations in mismatch repair genes are frequent in colorectal cancer after Hodgkin's lymphoma treatment.

Lisanne S Rigter ,
Petur Snaebjornsson ,
Efraim H Rosenberg ,
Peggy N Atmodimedjo ,
Berthe M Aleman ,
Jelle Ten Hoeve ,
Willemina R Geurts-Giele ,
,
Thomas W van Ravesteyn ,
Johan Hoeksel ,
Gerrit A Meijer ,
Hein Te Riele ,
Flora E van Leeuwen ,
Winand N Dinjens ,
Monique E van Leerdam

Abstract

CONCLUSIONS

We have demonstrated a higher frequency of MSI among t-CRCs, which results from somatic MMR gene mutations. This suggests a novel association of somatic MMR gene mutations with prior anticancer treatment.

RESULTS

KRAS and BRAF mutations were present in 41% and 15% t-CRCs, respectively. Compared with CRCs in the general population, t-CRCs had a higher MSI frequency (24% vs 11%, p=0.003) and more frequent loss of MSH2/MSH6 staining (13% vs 1%, p<0.001). Loss of MLH1/PMS2 staining and MLH1 promoter methylation were equally common in t-CRCs and the general population. In MSI CRCs without MLH1 promoter methylation, double somatic MMR gene mutations (or loss of heterozygosity as second hit) were detected in 7/10 (70%) t-CRCs and 8/36 (22%) CRCs in the general population (p=0.008). These MMR gene mutations in t-CRCs were classified as pathogenic. MSI t-CRC cases could not be ascribed to Lynch syndrome.

DESIGN

54 t-CRCs diagnosed in a Hodgkin's lymphoma survivor cohort were analysed for mismatch repair (MMR) proteins by immunohistochemistry, microsatellite instability (MSI) and KRAS/BRAF mutations. MSI t-CRCs were evaluated for promoter methylation and mutations in MMR genes. Pathogenicity of MMR gene mutations was evaluated by in silico predictions and functional analyses. Frequencies were compared with a general population cohort of CRC (n=1111).

OBJECTIVE

Hodgkin's lymphoma survivors who were treated with infradiaphragmatic radiotherapy or procarbazine-containing chemotherapy have a fivefold increased risk of developing colorectal cancer (CRC). This study aims to provide insight into the development of therapy-related CRC (t-CRC) by evaluating histopathological and molecular characteristics.

More about this publication

Gut

Volume 67
Issue nr. 3
Pages 447-455
Publication date 01-03-2018

Full text links

Publisher website (DOI) 10.1136/gutjnl-2016-312608
Europe PubMed Central 29439113
Pubmed 29439113

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