New Topoisomerase I mutations are associated with resistance to camptothecin

BACKGROUND: Topoisomerase I (TOP1) is a nuclear enzyme that catalyzes the relaxation of supercoiled DNA during DNA replication and transcription. TOP1 is the molecular target of camptothecin and related drugs such as irinotecan and SN38 (irinotecan's active metabolite). Irinotecan is widely use...

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Autores principales: Gongora, Céline, Vezzio-Vie, Nadia, Tuduri, Sandie, Denis, Vincent, Causse, Annick, Auzanneau, Céline, Collod-Beroud, Gwenaëlle, Coquelle, Arnaud, Pasero, Philippe, Pourquier, Philippe, Martineau, Pierre, Del Rio, Maguy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3120799/
https://www.ncbi.nlm.nih.gov/pubmed/21619602
http://dx.doi.org/10.1186/1476-4598-10-64
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author Gongora, Céline
Vezzio-Vie, Nadia
Tuduri, Sandie
Denis, Vincent
Causse, Annick
Auzanneau, Céline
Collod-Beroud, Gwenaëlle
Coquelle, Arnaud
Pasero, Philippe
Pourquier, Philippe
Martineau, Pierre
Del Rio, Maguy
author_facet Gongora, Céline
Vezzio-Vie, Nadia
Tuduri, Sandie
Denis, Vincent
Causse, Annick
Auzanneau, Céline
Collod-Beroud, Gwenaëlle
Coquelle, Arnaud
Pasero, Philippe
Pourquier, Philippe
Martineau, Pierre
Del Rio, Maguy
author_sort Gongora, Céline
collection PubMed
description BACKGROUND: Topoisomerase I (TOP1) is a nuclear enzyme that catalyzes the relaxation of supercoiled DNA during DNA replication and transcription. TOP1 is the molecular target of camptothecin and related drugs such as irinotecan and SN38 (irinotecan's active metabolite). Irinotecan is widely used as an anti-cancer agent in the treatment of metastatic colon cancer. However, its efficacy is often limited by the development of resistance. METHODS: We previously established several SN38 resistant HCT116-derived clones to study the mechanisms underlying resistance to SN38. Here, we investigated whether resistance to SN38 in these cell lines could be linked to the presence of TOP1 mutations and changes in its expression and activity. Functional analyses were performed on these cell lines challenged with SN38 and we specifically monitored the double strands breaks with γH2AX staining and replication activity with molecular combing. RESULTS: In SN38 resistant HCT116 clones we identified three new TOP1 mutations, which are located in the core subdomain III (p.R621H and p.L617I) and in the linker domain (p.E710G) and are packed together at the interface between these two domains. The presence of these TOP1 mutations in SN38 resistant HCT116 cells did not modify TOP1 expression or intrinsic activity. Conversely, following challenge with SN38, we observed a decrease of TOP1-DNA cleavage complexes and a reduction in double-stranded break formation). In addition, we showed that SN38 resistant HCT116 cells present a strong decrease in the SN38-dependent asymmetry of replication forks that is characteristic of SN38 sensitive HCT116 cells. CONCLUSIONS: These results indicate that the TOP1 mutations are involved in the development of SN38 resistance. We hypothesize that p.L617, p.R621 and p.E710 TOP1 residues are important for the functionality of the linker and that mutation of one of these residues is sufficient to alter or modulate its flexibility. Consequently, linker fluctuations could have an impact on SN38 binding by reducing the enzyme affinity for the drug.
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spelling pubmed-31207992011-06-23 New Topoisomerase I mutations are associated with resistance to camptothecin Gongora, Céline Vezzio-Vie, Nadia Tuduri, Sandie Denis, Vincent Causse, Annick Auzanneau, Céline Collod-Beroud, Gwenaëlle Coquelle, Arnaud Pasero, Philippe Pourquier, Philippe Martineau, Pierre Del Rio, Maguy Mol Cancer Research BACKGROUND: Topoisomerase I (TOP1) is a nuclear enzyme that catalyzes the relaxation of supercoiled DNA during DNA replication and transcription. TOP1 is the molecular target of camptothecin and related drugs such as irinotecan and SN38 (irinotecan's active metabolite). Irinotecan is widely used as an anti-cancer agent in the treatment of metastatic colon cancer. However, its efficacy is often limited by the development of resistance. METHODS: We previously established several SN38 resistant HCT116-derived clones to study the mechanisms underlying resistance to SN38. Here, we investigated whether resistance to SN38 in these cell lines could be linked to the presence of TOP1 mutations and changes in its expression and activity. Functional analyses were performed on these cell lines challenged with SN38 and we specifically monitored the double strands breaks with γH2AX staining and replication activity with molecular combing. RESULTS: In SN38 resistant HCT116 clones we identified three new TOP1 mutations, which are located in the core subdomain III (p.R621H and p.L617I) and in the linker domain (p.E710G) and are packed together at the interface between these two domains. The presence of these TOP1 mutations in SN38 resistant HCT116 cells did not modify TOP1 expression or intrinsic activity. Conversely, following challenge with SN38, we observed a decrease of TOP1-DNA cleavage complexes and a reduction in double-stranded break formation). In addition, we showed that SN38 resistant HCT116 cells present a strong decrease in the SN38-dependent asymmetry of replication forks that is characteristic of SN38 sensitive HCT116 cells. CONCLUSIONS: These results indicate that the TOP1 mutations are involved in the development of SN38 resistance. We hypothesize that p.L617, p.R621 and p.E710 TOP1 residues are important for the functionality of the linker and that mutation of one of these residues is sufficient to alter or modulate its flexibility. Consequently, linker fluctuations could have an impact on SN38 binding by reducing the enzyme affinity for the drug. BioMed Central 2011-05-27 /pmc/articles/PMC3120799/ /pubmed/21619602 http://dx.doi.org/10.1186/1476-4598-10-64 Text en Copyright ©2011 Gongora 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
Gongora, Céline
Vezzio-Vie, Nadia
Tuduri, Sandie
Denis, Vincent
Causse, Annick
Auzanneau, Céline
Collod-Beroud, Gwenaëlle
Coquelle, Arnaud
Pasero, Philippe
Pourquier, Philippe
Martineau, Pierre
Del Rio, Maguy
New Topoisomerase I mutations are associated with resistance to camptothecin
title New Topoisomerase I mutations are associated with resistance to camptothecin
title_full New Topoisomerase I mutations are associated with resistance to camptothecin
title_fullStr New Topoisomerase I mutations are associated with resistance to camptothecin
title_full_unstemmed New Topoisomerase I mutations are associated with resistance to camptothecin
title_short New Topoisomerase I mutations are associated with resistance to camptothecin
title_sort new topoisomerase i mutations are associated with resistance to camptothecin
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3120799/
https://www.ncbi.nlm.nih.gov/pubmed/21619602
http://dx.doi.org/10.1186/1476-4598-10-64
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