Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy

BACKGROUND: In previous analyses we identified therapy-induced upregulation of the CDK inhibitor p21(CIP/WAF-1 )and consequently decreased tumor cell proliferation or loss of Bax as adverse factors for survival in rectal cancer treated with radiochemotherapy. Here, we address the individual role of...

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Autores principales: Sturm, Isrid, Rau, Beate, Schlag, Peter M, Wust, Peter, Hildebrandt, Bert, Riess, Hanno, Hauptmann, Steffen, Dörken, Bernd, Daniel, Peter T
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1525199/
https://www.ncbi.nlm.nih.gov/pubmed/16686938
http://dx.doi.org/10.1186/1471-2407-6-124
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author Sturm, Isrid
Rau, Beate
Schlag, Peter M
Wust, Peter
Hildebrandt, Bert
Riess, Hanno
Hauptmann, Steffen
Dörken, Bernd
Daniel, Peter T
author_facet Sturm, Isrid
Rau, Beate
Schlag, Peter M
Wust, Peter
Hildebrandt, Bert
Riess, Hanno
Hauptmann, Steffen
Dörken, Bernd
Daniel, Peter T
author_sort Sturm, Isrid
collection PubMed
description BACKGROUND: In previous analyses we identified therapy-induced upregulation of the CDK inhibitor p21(CIP/WAF-1 )and consequently decreased tumor cell proliferation or loss of Bax as adverse factors for survival in rectal cancer treated with radiochemotherapy. Here, we address the individual role of p53 and its transcriptional targets, p21(CIP/WAF-1 )and Bax, on apoptosis induced by individual components of multimodal anticancer therapy, i.e. 5-fluorouracil (5-FU), ionising γ-radiation (IR) and heat shock/hyperthermia. METHODS: We analysed tumor samples 66 patients with rectal carcinoma treated by a neoadjuvant approach with radiochemotherapy ± heat shock/hyperthermia for the expression and mutation of p53 and the expression of p21(CIP/WAF-1 )and Bax. These data were correlated with the tumor response. The functional relevance of p53, p21(CIP/WAF-1 )and Bax was investigated in isogeneic HCT116 cell mutants treated with 5-FU, IR and heat shock. RESULTS: Rectal carcinoma patients who received an optimal heat shock treatment showed a response that correlated well with Bax expression (p = 0.018). Local tumor response in the whole cohort was linked to expression of p21(CIP/WAF-1 )(p < 0.05), but not p53 expression or mutation. This dichotomy of p53 pathway components regulating response to therapy was confirmed in vitro. In isogeneic HCT116 cell mutants, loss of Bax but not p53 or p21(CIP/WAF-1 )resulted in resistance against heat shock. In contrast, loss of p21(CIP/WAF-1 )or, to a lesser extent, p53 sensitized predominantly for 5-FU and IR. CONCLUSION: These data establish a different impact of p53 pathway components on treatment responses. While chemotherapy and IR depend primarily on cell cycle control and p21, heat shock depends primarily on Bax. In contrast, p53 status poorly correlates with response. These analyses therefore provide a rational approach for dissecting the mode of action of single treatment modalities that may be employed to circumvent clinically relevant resistance mechanisms in rectal cancer.
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spelling pubmed-15251992006-08-02 Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy Sturm, Isrid Rau, Beate Schlag, Peter M Wust, Peter Hildebrandt, Bert Riess, Hanno Hauptmann, Steffen Dörken, Bernd Daniel, Peter T BMC Cancer Research Article BACKGROUND: In previous analyses we identified therapy-induced upregulation of the CDK inhibitor p21(CIP/WAF-1 )and consequently decreased tumor cell proliferation or loss of Bax as adverse factors for survival in rectal cancer treated with radiochemotherapy. Here, we address the individual role of p53 and its transcriptional targets, p21(CIP/WAF-1 )and Bax, on apoptosis induced by individual components of multimodal anticancer therapy, i.e. 5-fluorouracil (5-FU), ionising γ-radiation (IR) and heat shock/hyperthermia. METHODS: We analysed tumor samples 66 patients with rectal carcinoma treated by a neoadjuvant approach with radiochemotherapy ± heat shock/hyperthermia for the expression and mutation of p53 and the expression of p21(CIP/WAF-1 )and Bax. These data were correlated with the tumor response. The functional relevance of p53, p21(CIP/WAF-1 )and Bax was investigated in isogeneic HCT116 cell mutants treated with 5-FU, IR and heat shock. RESULTS: Rectal carcinoma patients who received an optimal heat shock treatment showed a response that correlated well with Bax expression (p = 0.018). Local tumor response in the whole cohort was linked to expression of p21(CIP/WAF-1 )(p < 0.05), but not p53 expression or mutation. This dichotomy of p53 pathway components regulating response to therapy was confirmed in vitro. In isogeneic HCT116 cell mutants, loss of Bax but not p53 or p21(CIP/WAF-1 )resulted in resistance against heat shock. In contrast, loss of p21(CIP/WAF-1 )or, to a lesser extent, p53 sensitized predominantly for 5-FU and IR. CONCLUSION: These data establish a different impact of p53 pathway components on treatment responses. While chemotherapy and IR depend primarily on cell cycle control and p21, heat shock depends primarily on Bax. In contrast, p53 status poorly correlates with response. These analyses therefore provide a rational approach for dissecting the mode of action of single treatment modalities that may be employed to circumvent clinically relevant resistance mechanisms in rectal cancer. BioMed Central 2006-05-10 /pmc/articles/PMC1525199/ /pubmed/16686938 http://dx.doi.org/10.1186/1471-2407-6-124 Text en Copyright © 2006 Sturm 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 cited.
spellingShingle Research Article
Sturm, Isrid
Rau, Beate
Schlag, Peter M
Wust, Peter
Hildebrandt, Bert
Riess, Hanno
Hauptmann, Steffen
Dörken, Bernd
Daniel, Peter T
Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
title Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
title_full Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
title_fullStr Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
title_full_unstemmed Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
title_short Genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
title_sort genetic dissection of apoptosis and cell cycle control in response of colorectal cancer treated with preoperative radiochemotherapy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1525199/
https://www.ncbi.nlm.nih.gov/pubmed/16686938
http://dx.doi.org/10.1186/1471-2407-6-124
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