Poor-prognosis colon cancer is defined by a molecularly distinct subtype and develops from serrated precursor lesions

Felipe de Sousa E Melo; Xin Wang; Marnix Jansen; Evelyn Fessler; Anne Trinh; Laura P. M. H. de Rooij; Joan H. de Jong; Onno J. de Boer; Ronald van Leersum; Maarten F. Bijlsma; Hans Rodermond; Maartje van der Heijden; Carel J. M. van Noesel; Jurriaan B. Tuynman; Evelien Dekker; Florian Markowetz; Jan Paul Medema; Louis Vermeulen

doi:https://doi.org/10.1038/nm.3174

Poor-prognosis colon cancer is defined by a molecularly distinct subtype and develops from serrated precursor lesions

Felipe de Sousa E Melo, Xin Wang, Marnix Jansen, Evelyn Fessler, Anne Trinh, Laura P. M. H. de Rooij, Joan H. de Jong, Onno J. de Boer, Ronald van Leersum, Maarten F. Bijlsma, Hans Rodermond, Maartje van der Heijden, Carel J. M. van Noesel, Jurriaan B. Tuynman, Evelien Dekker, Florian Markowetz, Jan Paul Medema, Louis Vermeulen

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

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Abstract

Colon cancer is a clinically diverse disease. This heterogeneity makes it difficult to determine which patients will benefit most from adjuvant therapy and impedes the development of new targeted agents. More insight into the biological diversity of colon cancers, especially in relation to clinical features, is therefore needed. We demonstrate, using an unsupervised classification strategy involving over 1,100 individuals with colon cancer, that three main molecularly distinct subtypes can be recognized. Two subtypes have been previously identified and are well characterized (chromosomal-instable and microsatellite-instable cancers). The third subtype is largely microsatellite stable and contains relatively more CpG island methylator phenotype-positive carcinomas but cannot be identified on the basis of characteristic mutations. We provide evidence that this subtype relates to sessile-serrated adenomas, which show highly similar gene expression profiles, including upregulation of genes involved in matrix remodeling and epithelial-mesenchymal transition. The identification of this subtype is crucial, as it has a very unfavorable prognosis and, moreover, is refractory to epidermal growth factor receptor-targeted therapy

Original language	English
Pages (from-to)	614-618
Journal	Nature medicine
Volume	19
Issue number	5
DOIs	https://doi.org/10.1038/nm.3174
Publication status	Published - 2013

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https://doi.org/10.1038/nm.3174

Cite this

de Sousa E Melo, F., Wang, X., Jansen, M., Fessler, E., Trinh, A., de Rooij, L. P. M. H., de Jong, J. H., de Boer, O. J., van Leersum, R., Bijlsma, M. F., Rodermond, H., van der Heijden, M., van Noesel, C. J. M., Tuynman, J. B., Dekker, E., Markowetz, F., Medema, J. P., & Vermeulen, L. (2013). Poor-prognosis colon cancer is defined by a molecularly distinct subtype and develops from serrated precursor lesions. Nature medicine, 19(5), 614-618. https://doi.org/10.1038/nm.3174

@article{f1406bbf84b7468ebeaebf33d198752e,

title = "Poor-prognosis colon cancer is defined by a molecularly distinct subtype and develops from serrated precursor lesions",

abstract = "Colon cancer is a clinically diverse disease. This heterogeneity makes it difficult to determine which patients will benefit most from adjuvant therapy and impedes the development of new targeted agents. More insight into the biological diversity of colon cancers, especially in relation to clinical features, is therefore needed. We demonstrate, using an unsupervised classification strategy involving over 1,100 individuals with colon cancer, that three main molecularly distinct subtypes can be recognized. Two subtypes have been previously identified and are well characterized (chromosomal-instable and microsatellite-instable cancers). The third subtype is largely microsatellite stable and contains relatively more CpG island methylator phenotype-positive carcinomas but cannot be identified on the basis of characteristic mutations. We provide evidence that this subtype relates to sessile-serrated adenomas, which show highly similar gene expression profiles, including upregulation of genes involved in matrix remodeling and epithelial-mesenchymal transition. The identification of this subtype is crucial, as it has a very unfavorable prognosis and, moreover, is refractory to epidermal growth factor receptor-targeted therapy",

author = "{de Sousa E Melo}, Felipe and Xin Wang and Marnix Jansen and Evelyn Fessler and Anne Trinh and {de Rooij}, {Laura P. M. H.} and {de Jong}, {Joan H.} and {de Boer}, {Onno J.} and {van Leersum}, Ronald and Bijlsma, {Maarten F.} and Hans Rodermond and {van der Heijden}, Maartje and {van Noesel}, {Carel J. M.} and Tuynman, {Jurriaan B.} and Evelien Dekker and Florian Markowetz and Medema, {Jan Paul} and Louis Vermeulen",

year = "2013",

doi = "https://doi.org/10.1038/nm.3174",

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de Sousa E Melo, F, Wang, X, Jansen, M, Fessler, E, Trinh, A, de Rooij, LPMH, de Jong, JH , de Boer, OJ, van Leersum, R, Bijlsma, MF , Rodermond, H , van der Heijden, M , van Noesel, CJM , Tuynman, JB , Dekker, E, Markowetz, F, Medema, JP & Vermeulen, L 2013, 'Poor-prognosis colon cancer is defined by a molecularly distinct subtype and develops from serrated precursor lesions', Nature medicine, vol. 19, no. 5, pp. 614-618. https://doi.org/10.1038/nm.3174

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AU - de Sousa E Melo, Felipe

AU - Wang, Xin

AU - Jansen, Marnix

AU - Fessler, Evelyn

AU - Trinh, Anne

AU - de Rooij, Laura P. M. H.

AU - de Jong, Joan H.

AU - de Boer, Onno J.

AU - van Leersum, Ronald

AU - Bijlsma, Maarten F.

AU - Rodermond, Hans

AU - van der Heijden, Maartje

AU - van Noesel, Carel J. M.

AU - Tuynman, Jurriaan B.

AU - Dekker, Evelien

AU - Markowetz, Florian

AU - Medema, Jan Paul

AU - Vermeulen, Louis

PY - 2013

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AB - Colon cancer is a clinically diverse disease. This heterogeneity makes it difficult to determine which patients will benefit most from adjuvant therapy and impedes the development of new targeted agents. More insight into the biological diversity of colon cancers, especially in relation to clinical features, is therefore needed. We demonstrate, using an unsupervised classification strategy involving over 1,100 individuals with colon cancer, that three main molecularly distinct subtypes can be recognized. Two subtypes have been previously identified and are well characterized (chromosomal-instable and microsatellite-instable cancers). The third subtype is largely microsatellite stable and contains relatively more CpG island methylator phenotype-positive carcinomas but cannot be identified on the basis of characteristic mutations. We provide evidence that this subtype relates to sessile-serrated adenomas, which show highly similar gene expression profiles, including upregulation of genes involved in matrix remodeling and epithelial-mesenchymal transition. The identification of this subtype is crucial, as it has a very unfavorable prognosis and, moreover, is refractory to epidermal growth factor receptor-targeted therapy

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DO - https://doi.org/10.1038/nm.3174

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