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Target gene mutational pattern in Lynch syndrome colorectal carcinomas according to tumour location and germline mutation

Title
Target gene mutational pattern in Lynch syndrome colorectal carcinomas according to tumour location and germline mutation
Type
Article in International Scientific Journal
Year
2015
Authors
Pinheiro, M
(Author)
Other
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Pinto, C
(Author)
Other
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Peixoto, A
(Author)
Other
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Veiga, I
(Author)
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Lopes, P
(Author)
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Baldaia, H
(Author)
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Seruca, R
(Author)
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Tomlinson, I
(Author)
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Kovac, M
(Author)
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Heinimann, K
(Author)
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Journal
Vol. 113
Pages: 686-692
ISSN: 0007-0920
Publisher: Springer Nature
Other information
Authenticus ID: P-00G-FXG
Abstract (EN): Background: We previously reported that the target genes in sporadic mismatch repair (MMR)-deficient colorectal carcinomas (CRCs) in the distal colon differ from those occurring elsewhere in the colon. This study aimed to compare the target gene mutational pattern in microsatellite instability (MSI) CRC from Lynch syndrome patients stratified by tumour location and germline mutation, as well as with that of sporadic disease. Methods: A series of CRC from Lynch syndrome patients was analysed for MSI in genes predicted to be selective MSI targets and known to be involved in several pathways of colorectal carcinogenesis. Results: The most frequently mutated genes belong to the TGF-beta superfamily pathway, namely ACVR2A and TGFBR2. A significantly higher frequency of target gene mutations was observed in CRC from patients with germline mutations in MLH1 or MSH2 when compared with MSH6. Mutations in microsatellite sequences (A)7 of BMPR2 and (A)8 of MSH3 were significantly more frequent in the distal CRC. Additionally, we observed differences in MSH3 and TGFBR2 mutational frequency between Lynch syndrome and sporadic MSI CRC regarding tumour location. Conclusions: Our results indicate that the pattern of genetic changes differs in CRC depending on tumour location and between Lynch syndrome and sporadic MSI CRC, suggesting that carcinogenesis can occur by different pathways even if driven by generalised MSI.
Language: English
Type (Professor's evaluation): Scientific
No. of pages: 7
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