FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients

PURPOSE: Because cytidine deaminase (CDA) is the key enzyme in gemcitabine metabolism, numerous studies have attempted to investigate impact of CDA status (i.e. genotype or phenotype) on clinical outcome. To date, data are still controversial because none of these studies has fully investigated geno...

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Autores principales: Serdjebi, Cindy, Gagnière, Johan, Desramé, Jérôme, Fein, Francine, Guimbaud, Rosine, François, Eric, André, Thierry, Seitz, Jean-François, Montérymard, Carole, Arsene, Dominique, Volet, Julien, Abakar-Mahamat, Abakar, Lecomte, Thierry, Guerin-Meyer, Véronique, Legoux, Jean-Louis, Deplanque, Gaël, Guillet, Pierre, Ciccolini, Joseph, Lepage, Côme, Dahan, Laetitia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4550302/
https://www.ncbi.nlm.nih.gov/pubmed/26308942
http://dx.doi.org/10.1371/journal.pone.0135907
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author Serdjebi, Cindy
Gagnière, Johan
Desramé, Jérôme
Fein, Francine
Guimbaud, Rosine
François, Eric
André, Thierry
Seitz, Jean-François
Montérymard, Carole
Arsene, Dominique
Volet, Julien
Abakar-Mahamat, Abakar
Lecomte, Thierry
Guerin-Meyer, Véronique
Legoux, Jean-Louis
Deplanque, Gaël
Guillet, Pierre
Ciccolini, Joseph
Lepage, Côme
Dahan, Laetitia
author_facet Serdjebi, Cindy
Gagnière, Johan
Desramé, Jérôme
Fein, Francine
Guimbaud, Rosine
François, Eric
André, Thierry
Seitz, Jean-François
Montérymard, Carole
Arsene, Dominique
Volet, Julien
Abakar-Mahamat, Abakar
Lecomte, Thierry
Guerin-Meyer, Véronique
Legoux, Jean-Louis
Deplanque, Gaël
Guillet, Pierre
Ciccolini, Joseph
Lepage, Côme
Dahan, Laetitia
author_sort Serdjebi, Cindy
collection PubMed
description PURPOSE: Because cytidine deaminase (CDA) is the key enzyme in gemcitabine metabolism, numerous studies have attempted to investigate impact of CDA status (i.e. genotype or phenotype) on clinical outcome. To date, data are still controversial because none of these studies has fully investigated genotype-phenotype CDA status, pharmacokinetics and clinical outcome relationships in gemcitabine-treated patients. Besides, most patients were treated with gemcitabine associated with other drugs, thus adding a confounding factor. We performed a multicenter prospective clinical trial in gemcitabine-treated patients which aimed at investigating the link between CDA deficiency on the occurrence of severe toxicities and on pharmacokinetics, and studying CDA genotype-phenotype relationships. EXPERIMENTAL DESIGN: One hundred twenty patients with resected pancreatic adenocarcinoma eligible for adjuvant gemcitabine monotherapy were enrolled in this study promoted and managed by the Fédération Francophone de Cancérologie Digestive. Toxicities were graded according to National Cancer Institute’s Common Terminology Criteria for Adverse Events Version 4. They were considered severe for grade ≥ 3, and early when occurring during the first eight weeks of treatment. CDA status was evaluated using a double approach: genotyping for 79A>C and functional testing. Therapeutic drug monitoring of gemcitabine and its metabolite were performed on the first course of gemcitabine. RESULTS: Five patients out of 120 (i.e., 4.6%) were found to be CDA deficient (i.e., CDA activity <1.3 U/mg), and only one among them experienced early severe hematological toxicity. There was no statistically significant difference in CDA activity between patients experiencing hematological severe toxicities (28.44%) and patients who tolerated the treatment (71.56%). CDA genetic analysis failed in evidencing an impact in terms of toxicities or in CDA activity. Regarding pharmacokinetics, a wide inter-individual variability has been observed in patients. CONCLUSION: This study, which included only 4.6% of CDA-deficient patients, failed in identifying CDA status as a predictive marker of toxicities with gemcitabine. A lack of statistical power because of smoothing effect of CDA variability as compared with real life conditions could explain this absence of impact. TRIAL REGISTRATION: ClinicalTrials.gov NCT01416662
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spelling pubmed-45503022015-09-01 FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients Serdjebi, Cindy Gagnière, Johan Desramé, Jérôme Fein, Francine Guimbaud, Rosine François, Eric André, Thierry Seitz, Jean-François Montérymard, Carole Arsene, Dominique Volet, Julien Abakar-Mahamat, Abakar Lecomte, Thierry Guerin-Meyer, Véronique Legoux, Jean-Louis Deplanque, Gaël Guillet, Pierre Ciccolini, Joseph Lepage, Côme Dahan, Laetitia PLoS One Research Article PURPOSE: Because cytidine deaminase (CDA) is the key enzyme in gemcitabine metabolism, numerous studies have attempted to investigate impact of CDA status (i.e. genotype or phenotype) on clinical outcome. To date, data are still controversial because none of these studies has fully investigated genotype-phenotype CDA status, pharmacokinetics and clinical outcome relationships in gemcitabine-treated patients. Besides, most patients were treated with gemcitabine associated with other drugs, thus adding a confounding factor. We performed a multicenter prospective clinical trial in gemcitabine-treated patients which aimed at investigating the link between CDA deficiency on the occurrence of severe toxicities and on pharmacokinetics, and studying CDA genotype-phenotype relationships. EXPERIMENTAL DESIGN: One hundred twenty patients with resected pancreatic adenocarcinoma eligible for adjuvant gemcitabine monotherapy were enrolled in this study promoted and managed by the Fédération Francophone de Cancérologie Digestive. Toxicities were graded according to National Cancer Institute’s Common Terminology Criteria for Adverse Events Version 4. They were considered severe for grade ≥ 3, and early when occurring during the first eight weeks of treatment. CDA status was evaluated using a double approach: genotyping for 79A>C and functional testing. Therapeutic drug monitoring of gemcitabine and its metabolite were performed on the first course of gemcitabine. RESULTS: Five patients out of 120 (i.e., 4.6%) were found to be CDA deficient (i.e., CDA activity <1.3 U/mg), and only one among them experienced early severe hematological toxicity. There was no statistically significant difference in CDA activity between patients experiencing hematological severe toxicities (28.44%) and patients who tolerated the treatment (71.56%). CDA genetic analysis failed in evidencing an impact in terms of toxicities or in CDA activity. Regarding pharmacokinetics, a wide inter-individual variability has been observed in patients. CONCLUSION: This study, which included only 4.6% of CDA-deficient patients, failed in identifying CDA status as a predictive marker of toxicities with gemcitabine. A lack of statistical power because of smoothing effect of CDA variability as compared with real life conditions could explain this absence of impact. TRIAL REGISTRATION: ClinicalTrials.gov NCT01416662 Public Library of Science 2015-08-26 /pmc/articles/PMC4550302/ /pubmed/26308942 http://dx.doi.org/10.1371/journal.pone.0135907 Text en © 2015 Serdjebi 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
Serdjebi, Cindy
Gagnière, Johan
Desramé, Jérôme
Fein, Francine
Guimbaud, Rosine
François, Eric
André, Thierry
Seitz, Jean-François
Montérymard, Carole
Arsene, Dominique
Volet, Julien
Abakar-Mahamat, Abakar
Lecomte, Thierry
Guerin-Meyer, Véronique
Legoux, Jean-Louis
Deplanque, Gaël
Guillet, Pierre
Ciccolini, Joseph
Lepage, Côme
Dahan, Laetitia
FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients
title FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients
title_full FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients
title_fullStr FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients
title_full_unstemmed FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients
title_short FFCD-1004 Clinical Trial: Impact of Cytidine Deaminase Activity on Clinical Outcome in Gemcitabine-Monotherapy Treated Patients
title_sort ffcd-1004 clinical trial: impact of cytidine deaminase activity on clinical outcome in gemcitabine-monotherapy treated patients
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4550302/
https://www.ncbi.nlm.nih.gov/pubmed/26308942
http://dx.doi.org/10.1371/journal.pone.0135907
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