Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity

BACKGROUND: Radiation is an effective anti-cancer therapy but leads to severe late radiation toxicity in 5%–10% of patients. Assuming that genetic susceptibility impacts this risk, we hypothesized that the cellular response of normal tissue to X-rays could discriminate patients with and without late...

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Autores principales: Svensson, J. Peter, Stalpers, Lukas J. A, Lange, Rebecca E. E. Esveldt–van, Franken, Nicolaas A. P, Haveman, Jaap, Klein, Binie, Turesson, Ingela, Vrieling, Harry, Giphart-Gassler, Micheline
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2006
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1626552/
https://www.ncbi.nlm.nih.gov/pubmed/17076557
http://dx.doi.org/10.1371/journal.pmed.0030422
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author Svensson, J. Peter
Stalpers, Lukas J. A
Lange, Rebecca E. E. Esveldt–van
Franken, Nicolaas A. P
Haveman, Jaap
Klein, Binie
Turesson, Ingela
Vrieling, Harry
Giphart-Gassler, Micheline
author_facet Svensson, J. Peter
Stalpers, Lukas J. A
Lange, Rebecca E. E. Esveldt–van
Franken, Nicolaas A. P
Haveman, Jaap
Klein, Binie
Turesson, Ingela
Vrieling, Harry
Giphart-Gassler, Micheline
author_sort Svensson, J. Peter
collection PubMed
description BACKGROUND: Radiation is an effective anti-cancer therapy but leads to severe late radiation toxicity in 5%–10% of patients. Assuming that genetic susceptibility impacts this risk, we hypothesized that the cellular response of normal tissue to X-rays could discriminate patients with and without late radiation toxicity. METHODS AND FINDINGS: Prostate carcinoma patients without evidence of cancer 2 y after curative radiotherapy were recruited in the study. Blood samples of 21 patients with severe late complications from radiation and 17 patients without symptoms were collected. Stimulated peripheral lymphocytes were mock-irradiated or irradiated with 2-Gy X-rays. The 24-h radiation response was analyzed by gene expression profiling and used for classification. Classification was performed either on the expression of separate genes or, to augment the classification power, on gene sets consisting of genes grouped together based on function or cellular colocalization. X-ray irradiation altered the expression of radio-responsive genes in both groups. This response was variable across individuals, and the expression of the most significant radio-responsive genes was unlinked to radiation toxicity. The classifier based on the radiation response of separate genes correctly classified 63% of the patients. The classifier based on affected gene sets improved correct classification to 86%, although on the individual level only 21/38 (55%) patients were classified with high certainty. The majority of the discriminative genes and gene sets belonged to the ubiquitin, apoptosis, and stress signaling networks. The apoptotic response appeared more pronounced in patients that did not develop toxicity. In an independent set of 12 patients, the toxicity status of eight was predicted correctly by the gene set classifier. CONCLUSIONS: Gene expression profiling succeeded to some extent in discriminating groups of patients with and without severe late radiotherapy toxicity. Moreover, the discriminative power was enhanced by assessment of functionally or structurally related gene sets. While prediction of individual response requires improvement, this study is a step forward in predicting susceptibility to late radiation toxicity.
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spelling pubmed-16265522006-11-01 Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity Svensson, J. Peter Stalpers, Lukas J. A Lange, Rebecca E. E. Esveldt–van Franken, Nicolaas A. P Haveman, Jaap Klein, Binie Turesson, Ingela Vrieling, Harry Giphart-Gassler, Micheline PLoS Med Research Article BACKGROUND: Radiation is an effective anti-cancer therapy but leads to severe late radiation toxicity in 5%–10% of patients. Assuming that genetic susceptibility impacts this risk, we hypothesized that the cellular response of normal tissue to X-rays could discriminate patients with and without late radiation toxicity. METHODS AND FINDINGS: Prostate carcinoma patients without evidence of cancer 2 y after curative radiotherapy were recruited in the study. Blood samples of 21 patients with severe late complications from radiation and 17 patients without symptoms were collected. Stimulated peripheral lymphocytes were mock-irradiated or irradiated with 2-Gy X-rays. The 24-h radiation response was analyzed by gene expression profiling and used for classification. Classification was performed either on the expression of separate genes or, to augment the classification power, on gene sets consisting of genes grouped together based on function or cellular colocalization. X-ray irradiation altered the expression of radio-responsive genes in both groups. This response was variable across individuals, and the expression of the most significant radio-responsive genes was unlinked to radiation toxicity. The classifier based on the radiation response of separate genes correctly classified 63% of the patients. The classifier based on affected gene sets improved correct classification to 86%, although on the individual level only 21/38 (55%) patients were classified with high certainty. The majority of the discriminative genes and gene sets belonged to the ubiquitin, apoptosis, and stress signaling networks. The apoptotic response appeared more pronounced in patients that did not develop toxicity. In an independent set of 12 patients, the toxicity status of eight was predicted correctly by the gene set classifier. CONCLUSIONS: Gene expression profiling succeeded to some extent in discriminating groups of patients with and without severe late radiotherapy toxicity. Moreover, the discriminative power was enhanced by assessment of functionally or structurally related gene sets. While prediction of individual response requires improvement, this study is a step forward in predicting susceptibility to late radiation toxicity. Public Library of Science 2006-10 2006-10-31 /pmc/articles/PMC1626552/ /pubmed/17076557 http://dx.doi.org/10.1371/journal.pmed.0030422 Text en © 2006 Svensson et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Svensson, J. Peter
Stalpers, Lukas J. A
Lange, Rebecca E. E. Esveldt–van
Franken, Nicolaas A. P
Haveman, Jaap
Klein, Binie
Turesson, Ingela
Vrieling, Harry
Giphart-Gassler, Micheline
Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity
title Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity
title_full Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity
title_fullStr Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity
title_full_unstemmed Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity
title_short Analysis of Gene Expression Using Gene Sets Discriminates Cancer Patients with and without Late Radiation Toxicity
title_sort analysis of gene expression using gene sets discriminates cancer patients with and without late radiation toxicity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1626552/
https://www.ncbi.nlm.nih.gov/pubmed/17076557
http://dx.doi.org/10.1371/journal.pmed.0030422
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