P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation

BACKGROUND: Metastatic melanoma represents a major clinical problem. Its incidence continues to rise in western countries and there are currently no curative treatments. While mutation of the P53 tumour suppressor gene is a common feature of many types of cancer, mutational inactivation of P53 in me...

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Autores principales: Avery-Kiejda, Kelly A, Bowden, Nikola A, Croft, Amanda J, Scurr, Lyndee L, Kairupan, Carla F, Ashton, Katie A, Talseth-Palmer, Bente A, Rizos, Helen, Zhang, Xu D, Scott, Rodney J, Hersey, Peter
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3120805/
https://www.ncbi.nlm.nih.gov/pubmed/21615965
http://dx.doi.org/10.1186/1471-2407-11-203
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author Avery-Kiejda, Kelly A
Bowden, Nikola A
Croft, Amanda J
Scurr, Lyndee L
Kairupan, Carla F
Ashton, Katie A
Talseth-Palmer, Bente A
Rizos, Helen
Zhang, Xu D
Scott, Rodney J
Hersey, Peter
author_facet Avery-Kiejda, Kelly A
Bowden, Nikola A
Croft, Amanda J
Scurr, Lyndee L
Kairupan, Carla F
Ashton, Katie A
Talseth-Palmer, Bente A
Rizos, Helen
Zhang, Xu D
Scott, Rodney J
Hersey, Peter
author_sort Avery-Kiejda, Kelly A
collection PubMed
description BACKGROUND: Metastatic melanoma represents a major clinical problem. Its incidence continues to rise in western countries and there are currently no curative treatments. While mutation of the P53 tumour suppressor gene is a common feature of many types of cancer, mutational inactivation of P53 in melanoma is uncommon; however, its function often appears abnormal. METHODS: In this study whole genome bead arrays were used to examine the transcript expression of P53 target genes in extracts from 82 melanoma metastases and 6 melanoma cell lines, to provide a global assessment of aberrant P53 function. The expression of these genes was also examined in extracts derived from diploid human melanocytes and fibroblasts. RESULTS: The results indicated that P53 target transcripts involved in apoptosis were under-expressed in melanoma metastases and melanoma cell lines, while those involved in the cell cycle were over-expressed in melanoma cell lines. There was little difference in the transcript expression of P53 target genes between cell lines with null/mutant P53 compared to those with wild-type P53, suggesting that altered expression in melanoma was not related to P53 status. Similarly, down-regulation of P53 by short-hairpin RNA (shRNA) had limited effect on P53 target gene expression in melanoma cells, whereas there were a large number of P53 target genes whose mRNA expression was significantly altered by P53 inhibition in melanocytes. Analysis of whole genome gene expression profiles indicated that the ability of P53 to regulate genes involved in the cell cycle was significantly reduced in melanoma cells. Moreover, inhibition of P53 in melanocytes induced changes in gene expression profiles that were characteristic of melanoma cells and resulted in increased proliferation. Conversely, knockdown of P53 in melanoma cells resulted in decreased proliferation. CONCLUSIONS: These results indicate that P53 target genes involved in apoptosis and cell cycle regulation are aberrantly expressed in melanoma and that this aberrant functional activity of P53 may contribute to the proliferation of melanoma.
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spelling pubmed-31208052011-06-23 P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation Avery-Kiejda, Kelly A Bowden, Nikola A Croft, Amanda J Scurr, Lyndee L Kairupan, Carla F Ashton, Katie A Talseth-Palmer, Bente A Rizos, Helen Zhang, Xu D Scott, Rodney J Hersey, Peter BMC Cancer Research Article BACKGROUND: Metastatic melanoma represents a major clinical problem. Its incidence continues to rise in western countries and there are currently no curative treatments. While mutation of the P53 tumour suppressor gene is a common feature of many types of cancer, mutational inactivation of P53 in melanoma is uncommon; however, its function often appears abnormal. METHODS: In this study whole genome bead arrays were used to examine the transcript expression of P53 target genes in extracts from 82 melanoma metastases and 6 melanoma cell lines, to provide a global assessment of aberrant P53 function. The expression of these genes was also examined in extracts derived from diploid human melanocytes and fibroblasts. RESULTS: The results indicated that P53 target transcripts involved in apoptosis were under-expressed in melanoma metastases and melanoma cell lines, while those involved in the cell cycle were over-expressed in melanoma cell lines. There was little difference in the transcript expression of P53 target genes between cell lines with null/mutant P53 compared to those with wild-type P53, suggesting that altered expression in melanoma was not related to P53 status. Similarly, down-regulation of P53 by short-hairpin RNA (shRNA) had limited effect on P53 target gene expression in melanoma cells, whereas there were a large number of P53 target genes whose mRNA expression was significantly altered by P53 inhibition in melanocytes. Analysis of whole genome gene expression profiles indicated that the ability of P53 to regulate genes involved in the cell cycle was significantly reduced in melanoma cells. Moreover, inhibition of P53 in melanocytes induced changes in gene expression profiles that were characteristic of melanoma cells and resulted in increased proliferation. Conversely, knockdown of P53 in melanoma cells resulted in decreased proliferation. CONCLUSIONS: These results indicate that P53 target genes involved in apoptosis and cell cycle regulation are aberrantly expressed in melanoma and that this aberrant functional activity of P53 may contribute to the proliferation of melanoma. BioMed Central 2011-05-27 /pmc/articles/PMC3120805/ /pubmed/21615965 http://dx.doi.org/10.1186/1471-2407-11-203 Text en Copyright ©2011 Avery-Kiejda 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
Avery-Kiejda, Kelly A
Bowden, Nikola A
Croft, Amanda J
Scurr, Lyndee L
Kairupan, Carla F
Ashton, Katie A
Talseth-Palmer, Bente A
Rizos, Helen
Zhang, Xu D
Scott, Rodney J
Hersey, Peter
P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
title P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
title_full P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
title_fullStr P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
title_full_unstemmed P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
title_short P53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
title_sort p53 in human melanoma fails to regulate target genes associated with apoptosis and the cell cycle and may contribute to proliferation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3120805/
https://www.ncbi.nlm.nih.gov/pubmed/21615965
http://dx.doi.org/10.1186/1471-2407-11-203
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