Your search keyword '"C. Narjoz"' showing total 58 results

1. Dépistage du déficit en alpha1-antitrypsine sur sang capillaire recueilli sur papier-filtre : bilan des 20 premiers mois

Author

Christine Lombard, C. Narjoz, C. Chapuis Cellier, Farid Zerimech, Jean-François Mornex, Philippe Joly, Marie-Françoise Odou, Malika Balduyck, Infections Virales et Pathologie Comparée - UMR 754 (IVPC), École pratique des hautes études (EPHE), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Université Claude Bernard Lyon 1 (UCBL), and Université de Lyon-Université de Lyon-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)

Subjects

Pulmonary and Respiratory Medicine, Gynecology, Emphysema, medicine.medical_specialty, business.industry, Chronic obstructive pulmonary disease, [SDV.MHEP.PSR]Life Sciences [q-bio]/Human health and pathology/Pulmonology and respiratory tract, Bronchiectasis, 03 medical and health sciences, 0302 clinical medicine, Dried blood spot testing, 030228 respiratory system, Alpha1-antitrypsin, Medicine, 030212 general & internal medicine, business

Abstract

Resume Introduction Sous-diagnostique, le deficit en alpha1- antitrypsine est un facteur de predisposition aux pathologies bronchopulmonaires. Nous rapportons ici les resultats d’un depistage cible chez des individus a la semiologie respiratoire pouvant relever de ce deficit. Methodes De mars 2016 a octobre 2017, les patients ont ete selectionnes et le sang capillaire preleve au cours d’une consultation chez un pneumologue, puis expedie au laboratoire pour la determination de la concentration, du phenotype et du genotype de l’alpha1-antitrypsine. Resultats En 20 mois, 3728 trousses ont ete demandees par 566 pneumologues et 718 prelevements envoyes (19 %) : parmi eux, 708 etaient analysables, dont 613 accompagnes de renseignements cliniques relatifs au statut bronchopulmonaire. Au sein des 708 prelevements, 70 % ne presentaient aucun phenotype associe a un deficit de l’alpha1- antitrypsine, 7 % presentaient un phenotype associe a un deficit severe et 23 % un phenotype associe a un deficit intermediaire. Cent huit porteurs d’au moins une copie de PI*Z, donc a risque hepatique, ont ete detectes. Conclusions Les resultats de ce programme de depistage du deficit en alpha1- antitrypsine sur sang capillaire seche refletent une amelioration du diagnostic precoce du deficit dans les pathologies pulmonaires et montrent l’interet d’une bonne adhesion des pneumologues a cette campagne.

Published

2020

2. [Screening for alpha1-antitrypsin deficiency using dried blood spot: Assessment of the first 20 months]

Author

C, Chapuis Cellier, C, Narjoz, F, Zerimech, M-F, Odou, P, Joly, C, Lombard, J-F, Mornex, and M, Balduyck

Subjects

Adult, Aged, 80 and over, Male, Adolescent, Genotype, DNA Mutational Analysis, Middle Aged, Bronchiectasis, Pulmonary Disease, Chronic Obstructive, Young Adult, Phenotype, Pulmonary Emphysema, alpha 1-Antitrypsin, alpha 1-Antitrypsin Deficiency, Humans, Mass Screening, Female, Genetic Predisposition to Disease, Dried Blood Spot Testing, France, Longitudinal Studies, Child, Aged, Program Evaluation

Abstract

Alpha1-antitrypsin deficiency is a predisposing factor for pulmonary disease and under-diagnosis is a significant problem. The results of a targeted screening in patients with respiratory symptoms possibly indicative of severe deficiency are reported here.Data were collected from March 2016 to October 2017 on patients who had a capillary blood sample collected during a consultation with a pulmonologist and sent to the laboratory for processing to determine alpha1-antitrypsin concentration, phenotype and possibly genotype.In 20 months, 3728 test kits were requested by 566 pulmonologists and 718 (19 %) specimens sent: among these, 708 were analyzable and 613 were accompanied by clinical information. Of the 708 samples, 70 % had no phenotype associated with quantitative alpha1- antitrypsin deficiency, 7 % had a phenotype associated with a severe deficiency and 23 % had a phenotype associated with an intermediate deficiency. One hundred and eight patients carried at least one PI*Z allele which is considered to be a risk factor for liver disease.The results of this targeted screening program for alpha1- antitrypsin deficiency using a dried capillary blood sample reflect improvement in early diagnosis of this deficiency in lung disease with good adherence of the pulmonologists to this awareness campaign.

Published

2020

3. Artificial increase of uracilemia during fluoropyrimidine treatment can lead to DPD deficiency misinterpretation

Author

C. Narjoz, E Gautier-Veyret, Nicolas Pallet, Fabienne Thomas, M.-C. Etienne-Grimaldi, Groupe de Pharmacologie Clinique Oncologique, M Maillard, Antonin Schmitt, M Launay, C Tron, V Haufroid, Bernard Royer, UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - (SLuc) Service de biochimie médicale, UCL - (SLuc) Centre de toxicologie clinique, and UCL - (SLuc) Centre de génétique médicale UCL

Subjects

Dihydropyrimidine Dehydrogenase Deficiency, business.industry, MEDLINE, Hematology, Bioinformatics, medicine.disease, Dihydropyrimidine dehydrogenase deficiency, Text mining, Oncology, Fluorouracil, medicine, Humans, business, Lead (electronics), Capecitabine, Dihydrouracil Dehydrogenase (NADP), medicine.drug

Abstract

Each year in France, >75 000 patients receive fluoropyrimidines, including 5-fluorouracil (5-FU) and its oral prodrug capecitabine (Xeloda), to treat digestive, breast and head and neck cancers.1 Among them, ∼20% will experience severe hematological and digestive toxicities and

Published

2021

4. Erratum à « Dépistage du déficit en alpha1-antitrypsine sur sang capillaire recueilli sur papier-filtre : bilan des 20 premiers mois » [Rev. Mal. Respir. 37 (2020) 633–43]

Author

Christine Lombard, C. Narjoz, Malika Balduyck, Farid Zerimech, Marie-Françoise Odou, Jean-François Mornex, Philippe Joly, and C. Chapuis Cellier

Subjects

Pulmonary and Respiratory Medicine

Published

2021

5. Prevention of severe toxicity of fluoropyrimidines-based chemotherapy due to DPD deficiency: External quality evaluation of uracil and dihydrouracil measurements in plasma

Author

J. Ciccolini, I. Anglard, C. Narjoz, A. Vassault, Bernard Royer, and Fabienne Thomas

Subjects

Oncology, Chemotherapy, medicine.medical_specialty, business.industry, medicine.medical_treatment, Biochemistry (medical), Clinical Biochemistry, Dihydrouracil, Uracil, General Medicine, Biochemistry, chemistry.chemical_compound, chemistry, Internal medicine, Medicine, business, Severe toxicity

Published

2019

6. Biologie moléculaire et prise en charge des patients atteints d’adénocarcinomes du poumon

Author

C. Narjoz, Hélène Blons, Aurélie Cazes, and Laure Gibault

Subjects

Pulmonary and Respiratory Medicine, biology, business.industry, Locally advanced, medicine.disease_cause, Cancer research, biology.protein, medicine, Non small cell, Epidermal growth factor receptor, KRAS, business, neoplasms, Tyrosine kinase

Abstract

The management of locally advanced and metastatic non-small cell lung cancer has been revolutionized thanks to recent progress in pathology and molecular biology. The first molecular subgroup is defined by activating mutations of the epidermal growth factor receptor (EGFR), and a dramatic response to specific tyrosine kinase inhibitors. Since then, multiple genetic alterations (KRAS, HER2, BRAF, PIK3CA, ALK, ROS, RET…) have been identified as potential target of novel therapies, and molecular profiling has become common practice. This review focus on the molecular alterations associated with non-small cell lung cancer, including molecular profiling and response to targeted therapies.

Published

2014

7. Interindividual variability in dabigatran and rivaroxaban exposure: contribution of ABCB1 genetic polymorphisms and interaction with clarithromycin

Author

P Beaune, Pascale Gaussem, Marie-Anne Loriot, Virginie Siguret, Michel Azizi, Patrick Mismetti, C. Narjoz, Isabelle Gouin-Thibault, Anne Blanchard, Xavier Delavenne, Christian Funck-Brentano, and Joe-Elie Salem

Subjects

Adult, Male, Heterozygote, ATP Binding Cassette Transporter, Subfamily B, Adolescent, Genotype, medicine.drug_class, 030204 cardiovascular system & hematology, Pharmacology, Dabigatran, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Pharmacokinetics, Rivaroxaban, Clarithromycin, Medicine, Cytochrome P-450 CYP3A, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, Alleles, Polymorphism, Genetic, business.industry, Anticoagulant, Homozygote, Area under the curve, Hematology, Middle Aged, Crossover study, 030220 oncology & carcinogenesis, Area Under Curve, Mutation, Cytochrome P-450 CYP3A Inhibitors, business, Pharmacogenetics, medicine.drug

Abstract

Essentials Rivaroxaban and dabigatran are substrates of the P-glycoprotein (P-gp) encoded by the ABCB1 gene. We tested the effect of ABCB1 polymorphisms and of a P-gp inhibitor on both drugs' pharmacokinetics. The ABCB1 genotype was not a clinically relevant determinant of both drugs' pharmacokinetics. Administration of P-gp inhibitors with dabigatran or rivaroxaban should be exercised with caution. SummaryBackground The direct oral anticoagulants (DOACs) dabigatran and rivaroxaban are both substrates of the P-glycoprotein (P-gp) transporter, encoded by the ABCB1 gene. Rivaroxaban is metabolized by cytochrome P450 A4 (CYP3A4). Interindividual variability in DOAC exposure and frequent P-gp-associated drug–drug interactions have been described in patients. Objective To assess the influence of ABCB1 polymorphisms on the pharmacokinetics of dabigatran and rivaroxaban, associated or not with clarithromycin, a P-gp and CYP3A4 inhibitor. Methods Sixty healthy male volunteers, selected according to ABCB1 genotype (20 homozygous mutated, 20 heterozygous mutated, and 20 wild-type for haplotype 2677-3435), were included in this randomized, two-center, crossover study. All received sequentially a single dose of dabigatran etexilate (300 mg) and rivaroxaban (40 mg) associated or not with clarithromycin. Peak plasma concentration and area under the curve (AUC) were compared across the three ABCB1 genotypes. The effect of clarithromycin on dabigatran or rivaroxaban pharmacokinetics was assessed. Results Interindividual coefficients of variation for AUC were 77% for dabigatran and 51% for rivaroxaban. ABCB1 genotype did not significantly affect drug pharmacokinetics: AUC ratios between mutant-allele carriers and wild-type volunteers were 1.27 (95% confidence interval [CI] 0.84–1.92) and 1.20 (95% CI 0.96–1.51) for dabigatran and rivaroxaban, respectively. Clarithromycin coadministration led to a two-fold increase in both drugs’ AUC, irrespective of ABCB1 genotype: ratios of geometric means were 2.0 (95% CI 1.15–3.60) and 1.94 (95% CI 1.42–2.63) for dabigatran and rivaroxaban, respectively. Conclusions ABCB1 genotype is not a significant determinant of interindividual variability in dabigatran and rivaroxaban pharmacokinetics. The levels of one drug did not predict the levels of the other. Coadministration of a P-gp/CYP3A4 inhibitor with dabigatran or rivaroxaban may warrant caution in patients at risk of overexposure.

Published

2016

8. Genetic diseases

Author

T. Inazu, T. Kawahara, H. Endou, N. Anzai, I. Sebesta, B. Stiburkova, K. Ichida, M. Hosoyamada, A. Testa, D. Leonardis, F. Catalano, A. Pisano, A. Mafrica, B. Spoto, M. C. Sanguedolce, R. M. Parlongo, G. Tripepi, M. Postorino, G. Enia, C. Zoccali, F. Mallamaci, M. Working Group, A. Luque de Pablos, V. Garcia-Nieto, J. C. Lopez-Menchero, E. Ramos-Trujillo, H. Gonzalez-Acosta, F. Claverie-Martin, M. Arsali, P. Demosthenous, L. Papazachariou, Y. Athanasiou, K. Voskarides, C. Deltas, A. Pierides, S. Lee, K. H. Jeong, C. Ihm, T. W. Lee, S. H. Lee, J. Y. Moon, J. G. Wi, H. J. Lee, E. Y. Kim, K. Rogacev, A. Friedrich, B. Hummel, J. Berg, A. Zawada, D. Fliser, J. Geisel, G. H. Heine, I. Brabcova, S. Dusilova-Sulkova, Z. Krejcik, V. Stranecky, K. Lipar, T. Marada, J. Stepankova, O. Viklicky, M. Buraczynska, P. Zukowski, W. Zaluska, A. Kuczmaszewska, A. Ksiazek, M. Gaggl, S. Weidner, M. Hofer, J. Kleinert, G. Fauler, M. Wallner, P. Kotanko, G. Sunder-Plassmann, E. Paschke, R. Heguilen, L. Albarracin, J. Politei, A. A. Liste, A. Bernasconi, E. Kusano, R. Russo, A. Pisani, G. Messalli, M. Imbriaco, L. Prikhodina, O. Ryzhkova, V. Polyakov, K. Lipkowska, D. Ostalska-Nowicka, M. Smiech, M. Jaroniec, K. Zaorska, W. Szaflarski, M. Nowicki, J. Zachwieja, G. D'arrigo, J. Moskowitz, S. Piret, A. Tashman, E. Velez, K. Lhotta, R. Thakker, J. Cox, J. Kingswood, J. Mbundi, G. Attard, U. Patel, A. Saggar, F. Elmslie, T. Doyle, A. Jansen, S. Jozwiak, E. Belousova, M. Frost, R. Kuperman, M. Bebin, B. Korf, R. Flamini, M. Kohrman, S. Sparagana, J. Wu, J. Ford, G. Shah, D. Franz, B. Zonnenberg, W. Cheung, S. Urva, J. Wang, C. Kingswood, K. Budde, T. Kofman, C. Narjoz, Q. Raimbourg, M. Roland, M.-A. Loriot, A. Karras, G. S. Hill, C. Jacquot, D. Nochy, E. Thervet, P. Jagodzinski, M. Mostowska, A. Oko, N. Nicolaou, S. Kevelam, M. Lilien, M. Oosterveld, R. Goldschmeding, A. Van Eerde, R. Pfundt, A. Sonnenberg, P. Ter Hal, N. Knoers, K. Renkema, T. Storm, R. Nielsen, E. Christensen, C. Frykholm, L. Tranebjaerg, H. Birn, P. Verroust, T. Neveus, B. Sundelin, J. M. Hertz, G. Holmstrom, K. Ericson, A. Fabris, D. Cremasco, A. Zambon, E. Muraro, M. Alessi, A. D'angelo, F. Anglani, D. Del Prete, A. Alkmim Teixeira, B. M. Quinto, C. Jose Rodrigues, A. Beltrame Ribeiro, M. Batista, A. Kerti, R. Csohany, A. Szabo, O. Arkossy, P. Sallai, V. Moriniere, V. Vega-Warner, O. Lakatos, T. Szabo, G. Reusz, K. Tory, M. Addis, E. Tosetto, C. Meloni, M. Ceol, R. Cristofaro, M. A. Melis, P. Vercelloni, G. Marra, S. Kaniuka, M. Nagel, W. Wolyniec, L. Obolonczyk, R. Swiatkowska-Stodulska, K. Sworczak, B. Rutkowski, C. Chen, L. Jiang, L. Chen, L. Fang, M. Mozes M., M. Boosi, L. Rosivall, G. Kokeny, R. Diana, O. Gross, T. Johanna, G. Rainer, C. Ayse, H. Henrik, M. Gerhard-Anton, M. Nabil, E. Intissar, H. Belge, J. Bloch, K. Dahan, Y. Pirson, P. Vanhille, and N. Demoulin

Subjects

Transplantation, Nephrology

Published

2012

9. Review article: the benefits of pharmacogenetics for improving thiopurine therapy in inflammatory bowel disease

Author

Xavier Roblin, C. Narjoz, Laurent Chouchana, P Beaune, and Marie-Anne Loriot

Subjects

Drug, Hepatology, medicine.diagnostic_test, biology, Thiopurine methyltransferase, business.industry, media_common.quotation_subject, Gastroenterology, Pharmacology, medicine.disease, Inflammatory bowel disease, Therapeutic drug monitoring, Methylenetetrahydrofolate reductase, biology.protein, Medicine, Pharmacology (medical), Dosing, business, Adverse effect, Pharmacogenetics, media_common

Abstract

Aliment Pharmacol Ther 2012; 35: 15–36 Summary Background Thiopurines represent an effective and widely prescribed therapy in inflammatory bowel disease (IBD). Concerns about toxicity, mainly resulting from a wide inter-individual variability in thiopurine metabolism, restrict their use. Optimal thiopurine dosing is challenging for preventing adverse drug reactions and improving clinical response. Aim To review efficacy and toxicity of thiopurines in IBD. To provide pharmacogenetic-based therapeutic recommendations. Methods We conducted a query on PubMed database using ‘inflammatory bowel disease’, ‘thiopurine’, ‘azathioprine’, ‘6-mercaptopurine’, ‘TPMT’, ‘pharmacogenetics’, ‘TDM’, and selected relevant articles, especially clinical studies. Results Thiopurine metabolism – key enzyme: thiopurine S-methyltransferase (TPMT) – modulates clinical response, as it results in production of the pharmacologically active and toxic metabolites, the thioguanine nucleotides (6-TGN). Adjusting dosage according to TPMT status and/or metabolite blood levels is recommended for optimising thiopurine therapy (e.g. improving response rate up to 30% or decreasing haematological adverse events of 25%). Other enzymes or transporters of interest, as inosine triphosphatase (ITPase), glutathione S-transferase (GST), xanthine oxidase (XO), aldehyde oxidase (AOX), methylene tetrahydrofolate reductase (MTHFR) and ATP-binding cassette sub-family C member 4 (ABCC4) are reviewed and discussed for clinical relevance. Conclusions Based on the literature data, we provide a therapeutic algorithm for thiopurines therapy with starting dose recommendations depending on TPMT status and thereafter dose adjustments according to five metabolite profiles identified with therapeutic drug monitoring (TDM). This algorithm allows a dosage individualisation to optimise the management of patients under thiopurine. Furthermore, identification of new pharmacogenetic biomarkers is promising for ensuring maximal therapeutic response to thiopurines with a minimisation of the risk for adverse events.

Published

2011

10. Dépistage au cabinet du pneumologue du déficit sévère en alpha1-antitrypsine : premier bilan

Author

Christine Lombard, C. Chapuis Cellier, Farid Zerimech, Malika Balduyck, A. Jabet, and C. Narjoz

Subjects

Pulmonary and Respiratory Medicine, 030213 general clinical medicine, 03 medical and health sciences, 0302 clinical medicine

Abstract

Introduction Malgre l’individualisation depuis une cinquantaine d’annees du deficit severe en alpha1-antitrypsine (A1AT) et de ses consequences hepato-pulmonaires, cette entite genetique reste sous diagnostiquee. Afin de tenter de remedier a cet etat de fait, le LFB a developpe un kit permettant de prelever du sang capillaire et de le deposer sur un papier–filtre a partir duquel il est possible de mesurer la concentration en A1AT et de la phenotyper [1] . Nous nous proposons de rapporter ici le bilan des 5 premiers mois d’utilisation de ce kit. Methodes Ce kit comporte la totalite du materiel necessaire au prelevement, a son depot et a son envoi a l’un des 3 laboratoires correspondant au lieu d’exercice du pneumologue. A la carte de prelevement est associe un papier–filtre sur lequel sont dessines 3 emplacements correspondant chacun a un depot de 30 μL de sang total. Sur cette meme carte un emplacement est reserve aux renseignements cliniques et demographiques. Resultats Cent vingt-cinq prelevements issus de 125 patients dont 56 % d’hommes, 60 % de non-fumeurs (66/111) et d’âge moyen 58,5 ans (14–89 ans) ont ete analyses entre le 1 er mars et le 1 er aout 2016. L’histoire clinique de 114 patients ayant ete documentee, il est apparu que 78 avaient un emphyseme, isole dans 39 cas. Bien que 26 prelevements (21 %) n’aient pas ete conformes aux exigences de la technique (remplissage incomplet du cercle), 120 ont ete doses en A1AT puis phenotypes. Une concentration moyenne de 1,28 ± 0,41 g/L en A1AT a ete observee au sein de cette population caracterisee phenotypiquement par la presence de 97 PIM, 1 PIFM, 10 PIMS, 1PIS, 8 PIMZ et de 3 patients avec un phenotype severement deficitaire, 2 PIZ et 1 PIMmalton. Ces 3 derniers patients presentaient egalement un emphyseme isole avec histoire familiale et representaient 2,5 % de cette population pour une prevalence du deficit en A1AT dans la population generale de 1/5000. Conclusion Meme si un complement d’informations semble necessaire pour ameliorer la qualite du prelevement, ces premiers resultats sont tres prometteurs quant a l’efficacite de cette methode de depistage du deficit en alpha1-antitrypsine a partir d’un prelevement effectue au cabinet du pneumologue.

Published

2017

11. Letter: TPMT activity and age in IBD patients - authors' reply

Author

Xavier Roblin, Laurent Chouchana, C. Narjoz, Philippe Beaune, and Marie-Anne Loriot

Subjects

medicine.medical_specialty, Hepatology, Thiopurine methyltransferase, biology, business.industry, Internal medicine, Gastroenterology, medicine, biology.protein, Pharmacology (medical), business

Published

2012

12. Rôle des variants APOL1 dans la survenue des complications drépanocytaires

Author

J. Pouchot, Jean-Antoine Ribeil, C. Narjoz, Marie Courbebaisse, Eric Thervet, Anne-Sophie Jannot, R. Korman, Marianne Delville, and Jean-Benoit Arlet

Subjects

Gastroenterology, Internal Medicine

Abstract

Introduction Les variants G1 et G2 du gene APOL1 conferent une resistance a la trypanosomiase chez les Africains. Il a ete demontre qu’ils augmentaient le risque de nephropathie glomerulaire chez des porteurs du VIH ou des hypertendus. Un role pejoratif sur la nephropathie drepanocytaire (ND) a recemment ete rapporte chez des drepanocytaires Americains. Nous avons etudie l’impact de ces variants sur l’atteinte renale drepanocytaire, mais egalement sur les autres complications de la maladie, chez des patients d’origine africaine. Patients et methodes Tous patients drepanocytaires adultes vus consecutivement en consultation dans deux centres Franciliens etaient genotypes pour le gene APOL1. La ND etait evaluee par le debit de filtration glomerulaire estime (DFGe) par la formule CKD-EPI, les ratio microalbuminurie et proteinurie/creatininurie. Les complications aigues et chroniques drepanocytaires etaient recueillies. L’association statistique entre chaque variable et les variants d’APOL1 etait determinee grâce a un test exact de Fisher pour les variables qualitatives et un test de Wilcoxon pour les variables quantitatives. Nous avons egalement teste l’association entre les variants d’APOL1 et les variations du DFG et de la fuite proteique urinaire en fonction de l’âge en utilisant un modele lineaire mixte. Une correction prenait en compte, dans cette analyse, le genotype drepanocytaire, l’utilisation d’hydroxyuree, IEC ou de sartan. Resultats Cent cinquante-deux drepanocytaires d’âge median 30,4 ans (IQR 24,3–36,4), dont 118 SS ou S-beta thalassemiques (78 %), etaient inclus. Dix (7 %) des patients etaient porteurs des polymorphismes homozygotes ou double-heterozygotes d’APOL1 (G1/G1, n = 3 ; G2/G2, n = 1 ; G1/G2, n = 6) et 52 patients (34 %) etaient heterozygotes. En comparant les variables recueillies a la derniere visite du patient, les patients avec variants homozygotes ou double-heterozygotes d’APOL1 avaient plus souvent une atteinte renale terminale (IRT) compares aux drepanocytaires ayant le gene sauvage (30 % vs 1 %, p Discussion Notre etude confirme, pour la premiere fois dans chez des patients drepanocytaires d’origine africaine, le role nefaste des variants homozygotes ou doubles heterozygotes d’APOL1 sur la ND. Ces variants ont pour consequence une apparition plus precoce et une evolution beaucoup plus grave de la nephropathie. Notre etude apporte egalement deux elements nouveaux : le tropisme purement renal de ce modificateur genetique et le pronostic renal defavorables du polymorphisme heterozytoge G2/WT par rapport au G1/WT. Conclusion La determination systematique des variants d’APOL1 chez le patient drepanocytaire pourrait etre utile pour offrir un suivi renal plus regulier et optimiser le traitement nephroprotecteur chez les patients homozygotes ou doubles heterozygotes. La question de l’allogreffe de moelle peut se poser chez ces patients drepanocytaires vu le pronostic renal sombre.

Published

2017

13. [Molecular profiling of non-small cell lung cancer]

Author

L, Gibault, A, Cazes, C, Narjoz, and H, Blons

Subjects

Lung Neoplasms, Carcinoma, Non-Small-Cell Lung, Gene Expression Profiling, Decision Trees, Mutation, Humans, Molecular Targeted Therapy

Abstract

The management of locally advanced and metastatic non-small cell lung cancer has been revolutionized thanks to recent progress in pathology and molecular biology. The first molecular subgroup is defined by activating mutations of the epidermal growth factor receptor (EGFR), and a dramatic response to specific tyrosine kinase inhibitors. Since then, multiple genetic alterations (KRAS, HER2, BRAF, PIK3CA, ALK, ROS, RET…) have been identified as potential target of novel therapies, and molecular profiling has become common practice. This review focus on the molecular alterations associated with non-small cell lung cancer, including molecular profiling and response to targeted therapies.

Published

2013

14. Review article: the benefits of pharmacogenetics for improving thiopurine therapy in inflammatory bowel disease

Author

L, Chouchana, C, Narjoz, P, Beaune, M-A, Loriot, and X, Roblin

Subjects

Dose-Response Relationship, Drug, Pharmacogenetics, Azathioprine, Practice Guidelines as Topic, Humans, Methyltransferases, Inflammatory Bowel Diseases, Thioguanine, Algorithms, Immunosuppressive Agents

Abstract

Thiopurines represent an effective and widely prescribed therapy in inflammatory bowel disease (IBD). Concerns about toxicity, mainly resulting from a wide inter-individual variability in thiopurine metabolism, restrict their use. Optimal thiopurine dosing is challenging for preventing adverse drug reactions and improving clinical response.To review efficacy and toxicity of thiopurines in IBD. To provide pharmacogenetic-based therapeutic recommendations.We conducted a query on PubMed database using 'inflammatory bowel disease', 'thiopurine', 'azathioprine', '6-mercaptopurine', 'TPMT', 'pharmacogenetics', 'TDM', and selected relevant articles, especially clinical studies.Thiopurine metabolism - key enzyme: thiopurine S-methyltransferase (TPMT) - modulates clinical response, as it results in production of the pharmacologically active and toxic metabolites, the thioguanine nucleotides (6-TGN). Adjusting dosage according to TPMT status and/or metabolite blood levels is recommended for optimising thiopurine therapy (e.g. improving response rate up to 30% or decreasing haematological adverse events of 25%). Other enzymes or transporters of interest, as inosine triphosphatase (ITPase), glutathione S-transferase (GST), xanthine oxidase (XO), aldehyde oxidase (AOX), methylene tetrahydrofolate reductase (MTHFR) and ATP-binding cassette sub-family C member 4 (ABCC4) are reviewed and discussed for clinical relevance.Based on the literature data, we provide a therapeutic algorithm for thiopurines therapy with starting dose recommendations depending on TPMT status and thereafter dose adjustments according to five metabolite profiles identified with therapeutic drug monitoring (TDM). This algorithm allows a dosage individualisation to optimise the management of patients under thiopurine. Furthermore, identification of new pharmacogenetic biomarkers is promising for ensuring maximal therapeutic response to thiopurines with a minimisation of the risk for adverse events.

Published

2011

15. Letter: thiopurine blood monitoring for patients with inflammatory bowel disease - authors' reply

Author

C. Narjoz, Marie-Anne Loriot, Xavier Roblin, Philippe Beaune, and Laurent Chouchana

Subjects

medicine.medical_specialty, Hepatology, Thiopurine methyltransferase, biology, business.industry, Gastroenterology, Neutropenia, medicine.disease, Inflammatory bowel disease, Bone marrow suppression, Internal medicine, Toxicity, medicine, biology.protein, Pharmacology (medical), Vitamin B12, Adverse effect, business, Pharmacogenetics

Abstract

SIRS, We read carefully the letter from Dr El-Matary regarding our review on the benefits of pharmacogenetics for improving thiopurine therapy in inflammatory bowel disease. 2 We agree that performing blood testing remain a matter of debate for the prevention of thiopurine toxicity. First, neutropenia, strongly linked to high 6-thioguanine nucleotide blood level, is a frequent and serious adverse event of thiopurine therapy, potentially lethal. It frequently occurs in the first months of therapy, starting from 2 weeks, mostly in thiopurine S-methyltransferase deficient patients. However, neutropenia can happen anytime during therapy, until 27 years in long-term follow-up. Moreover, as Connell et al. showed, blood count is often normal, 1 month before the occurrence of a moderate or severe leucopenia. Nevertheless, this suggests that performing blood counts in a 3 months basis may have limited efficacy to predict early bone marrow suppression. Actually, early neutropenia probably differs from delayed toxicity, in which a dosage alteration, a therapy change or a deficiency in vitamin B12 or folates can be involved. Second, hepatotoxicity, probably related to elevated and lasting 6-methylmercaptopurine blood level, is commonly represented as mild, transient or reversible, elevation in serum transaminase. Thiopurine-induced liver injury occurs more frequently within the first months of treatment between, 1.5 and 5 months, although it can also occur after long-term treatment. 7 Thus, despite no consensus, liver tests can be easily added to routine blood count determinations. A recent meta-analysis did not conclude for clear benefits to maintain thiopurine therapy after 18 months. However, relapse occurs between 14% and 41% for the first subsequent year after therapy cessation. 10 In this meta-analysis, as the authors acknowledged, only two studies with high heterogeneity and poor statistical power were included for the assessment of relapse until 5 years. Finally, stopping an effective and well-tolerated thiopurine therapy is still questionable.

Published

2012

16. Role of CYP2D6 polymorphisms in tramadol metabolism in a context of co-medications and overweight.

Author

Ferron PJ, Pelletier R, Massart J, Narjoz C, Tran VJ, Loriot MA, Kernalleguen A, Zins M, Kab S, Morel I, Clément B, Gicquel T, and Le Daré B

Subjects

Humans, Female, Male, Middle Aged, Adult, Aged, Drug Interactions, Tramadol metabolism, Tramadol pharmacokinetics, Cytochrome P-450 CYP2D6 genetics, Cytochrome P-450 CYP2D6 metabolism, Polymorphism, Genetic, Analgesics, Opioid metabolism, Analgesics, Opioid pharmacokinetics, Overweight metabolism, Overweight genetics

Abstract

Very few quantitative data exist on tramadol metabolites, which hampers our understanding of their role in efficacy and safety of tramadol. We aimed to provide quantitative data on tramadol and its 5 main metabolites in a patient cohort and to determine whether metabolite ratios can be predictive of a CYP2D6 metabolism phenotype. We also aimed to investigate the influence of co-medications and patient profile (BMI, glycemia, lipid levels) on tramadol metabolite ratios. Overall, 37 patient samples from the CONSTANCES cohort contained tramadol and its 5 metabolites. Mean concentrations found tramadol at 343.2 ± 223.2 μg/L, M1 at 62.4 ± 41.4 μg/L, M2 at 210.0 ± 272.3, M3 at 1.76 ± 3.0 μg/L, M4 at 1.8 ± 2.8 μg/L and M5 at 31.8 ± 28.4 μg/L. The most frequent CYP2D6 phenotype was extensive metabolizers (51.3%), followed by intermediate metabolizers (24.3%) and poor metabolizers (10.8%). CYP2D6-inhibiting co-medications impacted tramadol metabolism independently of CYP2D6 metabolism phenotype. Lipid parameters and glycemia were significantly associated with changes in tramadol metabolic ratios. Metabolic ratios are not sufficient to determine the CYP2D6 metabolic phenotype in patients. CYP2D6 inhibitors and obesity/NAFLD/diabetes impact tramadol metabolism. These factors are likely to impact the analgesic efficacy and safety profile of tramadol, justifying the need for further studies in this area., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2025

17. A fatal case of 5-FU toxicity despite dose adjustment in a patient with a partial DPD deficiency receiving the FLOT regimen.

Author

Zaanan A, Pallet N, Narjoz C, Loriot MA, and Hafliger É

Subjects

Humans, Antimetabolites, Antineoplastic adverse effects, Antimetabolites, Antineoplastic administration & dosage, Antineoplastic Combined Chemotherapy Protocols adverse effects, Fatal Outcome, Dihydropyrimidine Dehydrogenase Deficiency complications, Fluorouracil administration & dosage, Fluorouracil adverse effects

Abstract

Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.

Published

2024

18. Diagnostic Yield of APOL1 p.N264K Variant Screening in Daily Practice.

Author

Narjoz C, Vinh-Hoang-Lan Julie Tran, Rabant M, Karras A, and Pallet N

Published

2024

19. Plasma lipidomic analysis to investigate putative biomarkers of P-glycoprotein activity in healthy volunteers.

Author

Decaix T, Magny R, Gouin-Thibaut I, Delavenne X, Mismetti P, Salem JE, Narjoz C, Blanchard A, Pépin M, Auzeil N, Loriot MA, and Laprévote O

Subjects

Humans, Healthy Volunteers, Biomarkers, ATP Binding Cassette Transporter, Subfamily B, Member 1 genetics, ATP Binding Cassette Transporter, Subfamily B genetics, Lipidomics, Clarithromycin pharmacology

Abstract

P-glycoprotein (P-gp) is an efflux transporter involved in the bioavailability of many drugs currently on the market. P-gp is responsible for several drug-drug interactions encountered in clinical practice leading to iatrogenic hospital admissions, especially in polypharmacy situations. ABCB1 genotyping only reflects an indirect estimate of P-gp activity. Therefore, it would be useful to identify endogenous biomarkers to determine the P-gp phenotype to predict in vivo activity prior to the initiation of treatment and to assess the effects of drugs on P-gp activity. The objective of this study was to assess changes in plasma lipidome composition among healthy volunteers selected on the basis of their ABCB1 genotype and who received clarithromycin, a known inhibitor of P-gp. Untargeted lipidomic analysis based on liquid chromatography-tandem mass spectrometry was performed before and after clarithromycin administration. Our results revealed changes in plasma levels of some ceramides (Cers) {Cer(d18:1/22:0), Cer(d18:1/22:1), and Cer(d18:1/20:0) by ~38% (p < 0.0001), 13% (p < 0.0001), and 13% (p < 0.0001), respectively} and phosphatidylcholines (PCs) {PC(17:0/14:1), PC(16:0/18:3), and PC(14:0/18:3) by ~24% (p < 0.001), 10% (p < 0.001), and 23.6% (p < 0.001)} associated with both ABCB1 genotype and clarithromycin intake. Through the examination of plasma lipids, our results highlight the relevance of untargeted lipidomics for studying in vivo P-gp activity and, more generally, to safely phenotyping transporters., (© 2023 The Authors. Clinical and Translational Science published by Wiley Periodicals LLC on behalf of American Society for Clinical Pharmacology and Therapeutics.)

Published

2023

20. Hydroxychloroquine sulfate: A novel treatment for lipin-1 deficiency?

Author

Renard P, Caccavelli L, Legendre A, Tuchmann-Durand C, Balakirouchenane D, Blanchet B, Narjoz C, Straube M, Hubas A, Garros A, Mention K, Bednarek N, Goudin N, Broissand C, Schlatter J, Cisternino S, Cagnard N, van Endert P, Diana J, de Calbiac H, and de Lonlay P

Subjects

Humans, Cytokines, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Phosphatidate Phosphatase genetics, Hydroxychloroquine pharmacology, Hydroxychloroquine therapeutic use, Quality of Life

Abstract

Background: Lipin-1 deficiency is a life-threatening disease that causes severe rhabdomyolysis (RM) and chronic symptoms associated with oxidative stress. In the absence of treatment, Hydroxychloroquine sulfate (HCQ) was administered to patients off label use on a compassionate basis in order to improve their physical conditions., Methods: Eleven patients with LPIN1 mutations were treated with HCQ. Clinical and biological efficacy and tolerance were assessed, including pain and quality of life, physical capacities, cardiopulmonary parameters, creatine kinase levels and plasma proinflammatory cytokines. To explore a dose-dependent effect of HCQ, primary myoblasts from 4 patients were incubated with various HCQ concentrations in growth medium (GM) or during starvation (EBSS medium) to investigate autophagy and oxidative stress., Findings: Under HCQ treatment, patient physical capacities improved. Abnormal cardiac function and peripheral muscle adaptation to exercise were normalized. However, two patients who had the highest mean blood HCQ concentrations experienced RM. We hypothesized that HCQ exerts deleterious effects at high concentrations by blocking autophagy, and beneficial effects on oxidative stress at low concentrations. We confirmed in primary myoblasts from 4 patients that high in vitro HCQ concentration (10 µM) but not low concentration (1 µM and 0.1 µM) induced autophagy blockage by modifying endolysosomal pH. Low HCQ concentration (1 µM) prevented reactive oxygen species (ROS) and oxidized DNA accumulation in myoblasts during starvation., Interpretation: HCQ improves the condition of patients with lipin-1 deficiency, but at low concentrations. In vitro, 1 µM HCQ decreases oxidative stress in myoblasts whereas higher concentrations have a deleterious effect by blocking autophagy., Competing Interests: Declaration of Competing Interest PVE and PDL have filed PCT (WO/2017/085115; EP3377095; PCT/EP2016/077843) and US patent applications (US20180325890). PVE and PDL have filed PCT (WO/2019/020732; PCT/EP2018/070256) patent applications. The remaining authors have no competing interests., (Copyright © 2023 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published

2023

21. Screening for dihydropyrimidine dehydrogenase deficiency by measuring uracilemia in chronic kidney disease patients is associated with a high rate of false positives.

Author

Narjoz C, Nadour Z, Zaanan A, Taieb J, Loriot MA, and Pallet N

Subjects

Humans, Dihydrouracil Dehydrogenase (NADP) genetics, Uracil, Glomerular Filtration Rate, Dihydropyrimidine Dehydrogenase Deficiency complications, Dihydropyrimidine Dehydrogenase Deficiency diagnosis, Renal Insufficiency, Chronic diagnosis, Renal Insufficiency, Chronic complications, Neoplasms complications

Abstract

Background: Pretherapeutic screening for dihydropyrimidine dehydrogenase (DPD) deficiency based on the measurement of plasma uracil ([U]) is recommended prior to the administration of fluoropyrimidine-based chemotherapy. Cancer patients frequently have impaired kidney function, but the extent to which kidney function decline impacts [U] levels has not been comprehensively investigated., Methods: We assessed the relationship between DPD phenotypes and estimated glomerular filtration rate (eGFR) in 1751 patients who benefited on the same day from a screening for DPD deficiency by measuring [U] and [UH 2 ]:[U], and an evaluation of eGFR. The impact of a kidney function decline on [U] levels and [UH 2 ]:[U] ratio was evaluated., Results: We observed that [U] was negatively correlated with eGFR, indicating that [U] levels increase as eGFR declines. For each ml/min of eGFR decrease, [U] value increased in average by 0.035 ng/ml. Using the KDIGO classification of chronic kidney disease (CKD), we observed that [U] values >16 ng/ml (DPD deficiency) were measured in 3.6 % and 4.4 % of stage 1 and 2 CKD (normal-high eGFR, >60 ml/min/1.73 m 2 ) patients, but in 6.7 % of stage 3A CKD patients (45 to 59 ml/min/1.73 m 2 ), 25% of stage 3B CKD patients (30 to 44 ml/min/1.73 m 2 ), 22.7% of stage 4 CKD patients (15 to 29 ml/min/1.73 m 2 and 26.7% of stage 5 CKD patients (<15 ml/min/1.73 m 2 ). [UH2]:[U] ratios were not impacted by kidney function., Conclusion: DPD phenotyping based on the measurement of plasma [U] in patients with decreased eGFR is associated with an exceedingly high rate of false positives when kidney function decline reaches 45 ml/minute/1.73 m 2 of eGFR or lower. In this population, an alternative strategy that remain to be evaluated would be to measure the [UH 2 ]:[U] ratio in addition to [U]., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier B.V. All rights reserved.)

Published

2023

22. Current diagnostic and clinical issues of screening for dihydropyrimidine dehydrogenase deficiency.

Author

Etienne-Grimaldi MC, Pallet N, Boige V, Ciccolini J, Chouchana L, Barin-Le Guellec C, Zaanan A, Narjoz C, Taieb J, Thomas F, and Loriot MA

Subjects

Humans, Fluorouracil, Antimetabolites, Antineoplastic therapeutic use, Capecitabine, Dihydrouracil Dehydrogenase (NADP) genetics, Dihydrouracil Dehydrogenase (NADP) metabolism, Dihydropyrimidine Dehydrogenase Deficiency complications, Dihydropyrimidine Dehydrogenase Deficiency diagnosis, Dihydropyrimidine Dehydrogenase Deficiency genetics

Abstract

Fluoropyrimidine drugs (FP) are the backbone of many chemotherapy protocols for treating solid tumours. The rate-limiting step of fluoropyrimidine catabolism is dihydropyrimidine dehydrogenase (DPD), and deficiency in DPD activity can result in severe and even fatal toxicity. In this review, we survey the evidence-based pharmacogenetics and therapeutic recommendations regarding DPYD (the gene encoding DPD) genotyping and DPD phenotyping to prevent toxicity and optimize dosing adaptation before FP administration. The French experience of mandatory DPD-deficiency screening prior to initiating FP is discussed., Competing Interests: Conflict of interest statement The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2023

23. Quantitative impact of pre-analytical process on plasma uracil when testing for dihydropyrimidine dehydrogenase deficiency.

Author

Maillard M, Launay M, Royer B, Guitton J, Gautier-Veyret E, Broutin S, Tron C, Le Louedec F, Ciccolini J, Richard D, Alarcan H, Haufroid V, Tafzi N, Schmitt A, Etienne-Grimaldi MC, Narjoz C, and Thomas F

Subjects

Humans, Dihydrouracil Dehydrogenase (NADP) genetics, Uracil, Phenotype, Plasma, Fluorouracil, Dihydropyrimidine Dehydrogenase Deficiency diagnosis

Abstract

Aims: Determining dihydropyrimidine dehydrogenase (DPD) activity by measuring patient's uracil (U) plasma concentration is mandatory before fluoropyrimidine (FP) administration in France. In this study, we aimed to refine the pre-analytical recommendations for determining U and dihydrouracil (UH 2 ) concentrations, as they are essential in reliable DPD-deficiency testing., Methods: U and UH 2 concentrations were collected from 14 hospital laboratories. Stability in whole blood and plasma after centrifugation, the type of anticoagulant and long-term plasma storage were evaluated. The variation induced by time and temperature was calculated and compared to an acceptability range of ±20%. Inter-occasion variability (IOV) of U and UH 2 was assessed in 573 patients double sampled for DPD-deficiency testing., Results: Storage of blood samples before centrifugation at room temperature (RT) should not exceed 1 h, whereas cold (+4°C) storage maintains the stability of uracil after 5 hours. For patients correctly double sampled, IOV of U reached 22.4% for U (SD = 17.9%, range = 0-99%). Notably, 17% of them were assigned with a different phenotype (normal or DPD-deficient) based on the analysis of their two samples. For those having at least one non-compliant sample, this percentage increased up to 33.8%. The moment of blood collection did not affect the DPD phenotyping result., Conclusion: Caution should be taken when interpreting U concentrations if the time before centrifugation exceeds 1 hour at RT, since it rises significantly afterwards. Not respecting the pre-analytical conditions for DPD phenotyping increases the risk of DPD status misclassification., (© 2022 The Authors. British Journal of Clinical Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society.)

Published

2023

24. Imbalance between alpha-1-antitrypsin and interleukin 6 is associated with in-hospital mortality and thrombosis during COVID-19.

Author

Philippe A, Puel M, Narjoz C, Gendron N, Durey-Dragon MA, Vedie B, Balduyck M, Chocron R, Hauw-Berlemont C, Sanchez O, Mirault T, Diehl JL, Smadja DM, and Loriot MA

Subjects

Humans, Cross-Sectional Studies, Inflammation, COVID-19 complications, COVID-19 mortality, Hospital Mortality, Interleukin-6 blood, alpha 1-Antitrypsin blood, Thrombosis virology

Abstract

Thrombosis is a hallmark of severe COVID-19. Alpha-1-antitrypsin (AAT), an inflammation-inducible serpin with anti-inflammatory, tissue protective and anticoagulant properties may be involved in severe COVID-19 pathophysiology including thrombosis onset. In this study, we examined AAT ability to predict occurrence of thrombosis and in-hospital mortality during COVID-19. To do so, we performed a monocentric cross-sectional study of 137 hospitalized patients with COVID-19 of whom 56 (41%) were critically ill and 33 (22.4%) suffered from thrombosis during hospitalization. We measured AAT and IL-6 plasma levels in all patients and phenotyped AAT in a subset of patients with or without thrombosis paired for age, sex and COVID-19 severity. We observed that AAT levels at admission were higher in both non-survivors and thrombosis patients than in survivors and non-thrombosis patients. AAT: IL-6 ratio was lower in non-survivors and thrombosis patients. In a logistic regression multivariable analysis model adjusted on age, BMI and D-dimer levels, a higher AAT: IL-6 was a protective factor of both in-hospital mortality (Odds ratio, OR: 0.07 95%CI [0.02-0.25], p < 0.001) and thrombosis (OR 0.36 95%CI [0.14-0.82], p = 0.02). AAT phenotyping did not show a higher proportion of AAT abnormal variants in thrombosis patients.Our findings suggest an insufficient production of AAT regarding inflammation intensity during severe COVID-19. AAT appeared as a powerful predictive marker of severity, mortality and thrombosis mirroring the imbalance between harmful inflammation and protective counter-balancing mechanism in COVID-19. Restoring the balance between AAT and inflammation could offer therapeutic opportunities in severe COVID-19., (Copyright © 2022. Published by Elsevier B.V.)

Published

2022

25. Exposure-Response Analysis of Osimertinib in Patients with Advanced Non-Small-Cell Lung Cancer.

Author

Rodier T, Puszkiel A, Cardoso E, Balakirouchenane D, Narjoz C, Arrondeau J, Fallet V, Khoudour N, Guidi M, Vidal M, Declèves X, Csajka C, Alexandre J, Cadranel J, Fabre E, Wislez M, Goldwasser F, and Blanchet B

Abstract

High interindividual variability (IIV) of the clinical response to epidermal growth factor receptor (EGFR) inhibitors such as osimertinib in non-small-cell lung cancer (NSCLC) might be related to the IIV in plasma exposure. The aim of this study was to evaluate the exposure−response relationship for toxicity and efficacy of osimertinib in unselected patients with advanced EGFR-mutant NSCLC. This retrospective analysis included 87 patients treated with osimertinib. Exposure−toxicity analysis was performed in the entire cohort and survival analysis only in second-line patients (n = 45). No significant relationship between occurrence of dose-limiting toxicity and plasma exposure was observed in the entire cohort (p = 0.23, n = 86). The median overall survival (OS) was approximately two-fold shorter in the 4th quartile (Q4) of osimertinib trough plasma concentration (>235 ng/mL) than in the Q1−Q3 group (12.2 months [CI95% = 8.0−not reached (NR)] vs. 22.7 months [CI95% = 17.1−34.1]), but the difference was not statistically significant (p = 0.15). To refine this result, the exposure−survival relationship was explored in a cohort of 41 NSCLC patients treated with erlotinib. The Q4 erlotinib exposure group (>1728 ng/mL) exhibited a six-fold shorter median OS than the Q1−Q3 group (4.8 months [CI95% = 3.3-NR] vs. 22.8 months (CI95% = 10.6−37.4), p = 0.00011). These results suggest that high exposure to EGFR inhibitors might be related to worse survival in NSCLC patients.

Published

2022

26. Pretherapeutic screening for Dihydropyrimidine deshydrogenase deficiency in measuring uracilemia in dialysis patients leads to a high rate of falsely positive results.

Author

Gaible C, Narjoz C, Loriot MA, Roueff S, and Pallet N

Subjects

Case-Control Studies, Dihydropyrimidine Dehydrogenase Deficiency enzymology, Dihydropyrimidine Dehydrogenase Deficiency etiology, False Positive Reactions, Follow-Up Studies, Humans, Kidney Failure, Chronic pathology, Prospective Studies, Dihydropyrimidine Dehydrogenase Deficiency diagnosis, Dihydrouracil Dehydrogenase (NADP) metabolism, Kidney Failure, Chronic therapy, Mass Screening methods, Renal Dialysis adverse effects, Uracil blood

Abstract

Background: Pretherapeutic screening for dihydropyrimidine dehydrogenase (DPD) deficiency is recommended prior to the administration of fluoropyrimidine-based chemotherapy. However, the best strategy to identify DPD deficiency in End Stage Renal Disease (ESRD) patients is unknown., Methods: We assessed the characteristics of both DPD phenotypes and DPYD genotypes in 20 dialyzed patients before and after dialysis session. The extent to which the concentrations of uracil [U] and dihydrouracil [UH 2 ] were affected by dialysis was evaluated., Results: Mean [U] was 14 ± 3.3 ng/ml before the dialysis session, and 7.9 ± 2.7 ng/ml after. Notably, mean [U] in 119 non-ESRD patients during the same timeline was 8.7 ± 3.9 ng/ml, which is similar to [U] values after dialysis session (p = 0.38). [U] values > 16 ng/ml were measured in 4 ESRD patients (20%), whereas the rate was 3.3% in the non-ESRD cohort. Whole gene sequencing did not reveal DPYD deleterious allelic variants in the 4 ESRD patients with [U] values > 16 ng/ml. The profile of [UH2] values during dialysis was similar to that of [U]: 385 ± 86 ng/ml before, and 185 ± 62 ng/ml after (mean reduction rate 42.5%). Thus, [UH2]:[U] ratio remained unaffected by dialysis, and was similar to the values in non-ESRD patients (22.4 ± 7.1)., Conclusion: Phenotyping based on measuring plasma [U] before a dialysis sessions in ESRD patients is associated with an unacceptable high rate of false positives. The optimal strategy for the identification of patients with DPD deficiency in this population would be the monitor the [UH 2 ]:[U] ratio, which remains unaffected., (© 2021. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2021

27. Identification of rare defective allelic variants in cases of thiopurine S-methyltransferase deficient activity.

Author

Chansavang A, Maalej S, Narjoz C, Loriot MA, and Pallet N

Subjects

Alleles, Exons, Genetic Variation, Genotype, High-Throughput Nucleotide Sequencing, Humans, Introns genetics, Mutation, Phenotype, Polymorphism, Genetic, Exome Sequencing, Methyltransferases deficiency, Methyltransferases genetics

Abstract

Aim: To assess rare TPMT variants in patients carrying a deficient phenotype not predicted by the four more frequent genotypes (*2, *3A, *3B and *3C ). Materials & methods: Next-generation sequencing of TPMT in 39 patients with a discordant genotype. Results: None of the variants identified explained the discordances assuming that they are of uncertain significance according to the Clinical Pharmacogenetics Implementation Consortium classification. Two unknown variants were detected and predicted to result in a splicing defect. We show that TPMT*16  and TMPT*21 are defective alleles, and TPMT*8 and TPMT*24 are associated with a normal activity. Conclusion: Whole-exon sequencing for rare  TPMT mutations has a low diagnostic yield. A reassessment of the functional impact of rare variants of uncertain significance is a critical issue.

Published

2020

28. [Screening for alpha1-antitrypsin deficiency using dried blood spot: Assessment of the first 20 months].

Author

Chapuis Cellier C, Narjoz C, Zerimech F, Odou MF, Joly P, Lombard C, Mornex JF, and Balduyck M

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Bronchiectasis blood, Bronchiectasis diagnosis, Bronchiectasis genetics, Child, DNA Mutational Analysis methods, DNA Mutational Analysis standards, Dried Blood Spot Testing standards, Female, France epidemiology, Genetic Predisposition to Disease, Genotype, Humans, Longitudinal Studies, Male, Mass Screening organization & administration, Middle Aged, Phenotype, Program Evaluation, Pulmonary Disease, Chronic Obstructive blood, Pulmonary Disease, Chronic Obstructive diagnosis, Pulmonary Disease, Chronic Obstructive genetics, Pulmonary Emphysema blood, Pulmonary Emphysema diagnosis, Pulmonary Emphysema genetics, Young Adult, alpha 1-Antitrypsin analysis, alpha 1-Antitrypsin genetics, alpha 1-Antitrypsin Deficiency blood, alpha 1-Antitrypsin Deficiency epidemiology, alpha 1-Antitrypsin Deficiency genetics, Dried Blood Spot Testing methods, Mass Screening methods, alpha 1-Antitrypsin Deficiency diagnosis

Abstract

Introduction: Alpha1-antitrypsin deficiency is a predisposing factor for pulmonary disease and under-diagnosis is a significant problem. The results of a targeted screening in patients with respiratory symptoms possibly indicative of severe deficiency are reported here., Methods: Data were collected from March 2016 to October 2017 on patients who had a capillary blood sample collected during a consultation with a pulmonologist and sent to the laboratory for processing to determine alpha1-antitrypsin concentration, phenotype and possibly genotype., Results: In 20 months, 3728 test kits were requested by 566 pulmonologists and 718 (19 %) specimens sent: among these, 708 were analyzable and 613 were accompanied by clinical information. Of the 708 samples, 70 % had no phenotype associated with quantitative alpha1- antitrypsin deficiency, 7 % had a phenotype associated with a severe deficiency and 23 % had a phenotype associated with an intermediate deficiency. One hundred and eight patients carried at least one PI*Z allele which is considered to be a risk factor for liver disease., Conclusions: The results of this targeted screening program for alpha1- antitrypsin deficiency using a dried capillary blood sample reflect improvement in early diagnosis of this deficiency in lung disease with good adherence of the pulmonologists to this awareness campaign., (Copyright © 2020 SPLF. Published by Elsevier Masson SAS. All rights reserved.)

Published

2020

29. A comprehensive population-based study comparing the phenotype and genotype in a pretherapeutic screen of dihydropyrimidine dehydrogenase deficiency.

Author

Pallet N, Hamdane S, Garinet S, Blons H, Zaanan A, Paillaud E, Taieb J, Laprevote O, Loriot MA, and Narjoz C

Subjects

Aged, Cohort Studies, Cross-Sectional Studies, Dihydropyrimidine Dehydrogenase Deficiency epidemiology, Dihydropyrimidine Dehydrogenase Deficiency genetics, Dihydrouracil Dehydrogenase (NADP) genetics, Dihydrouracil Dehydrogenase (NADP) metabolism, Female, France epidemiology, Genotype, High-Throughput Nucleotide Sequencing, Humans, Male, Middle Aged, Phenotype, Prevalence, Retrospective Studies, Uracil analogs & derivatives, Uracil blood, Uracil metabolism, Dihydropyrimidine Dehydrogenase Deficiency diagnosis

Abstract

Background: Pretherapeutic screening for dihydropyrimidine dehydrogenase (DPD) deficiency is recommended or required prior to the administration of fluoropyrimidine-based chemotherapy. However, the best strategy to identify DPD-deficient patients remains elusive., Methods: Among a nationwide cohort of 5886 phenotyped patients with cancer who were screened for DPD deficiency over a 3 years period, we assessed the characteristics of both DPD phenotypes and DPYD genotypes in a subgroup of 3680 patients who had completed the two tests. The extent to which defective allelic variants of DPYD predict DPD activity as estimated by the plasma concentrations of uracil [U] and its product dihydrouracil [UH 2 ] was evaluated., Results: When [U] was used to monitor DPD activity, 6.8% of the patients were classified as having DPD deficiency ([U] > 16 ng/ml), while the [UH 2 ]:[U] ratio identified 11.5% of the patients as having DPD deficiency (UH 2 ]:[U] < 10). [U] classified two patients (0.05%) with complete DPD deficiency (> 150 ng/ml), and [UH 2 ]:[U] < 1 identified three patients (0.08%) with a complete DPD deficiency. A defective DPYD variant was present in 4.5% of the patients, and two patients (0.05%) carrying 2 defective variants of DPYD were predicted to have low metabolism. The mutation status of DPYD displayed a very low positive predictive value in identifying individuals with DPD deficiency, although a higher predictive value was observed when [UH 2 ]:[U] was used to measure DPD activity. Whole exon sequencing of the DPYD gene in 111 patients with DPD deficiency and a "wild-type" genotype (based on the four most common variants) identified seven heterozygous carriers of a defective allelic variant., Conclusions: Frequent genetic DPYD variants have low performances in predicting partial DPD deficiency when evaluated by [U] alone, and [UH 2 ]:[U] might better reflect the impact of genetic variants on DPD activity. A clinical trial comparing toxicity rates after dose adjustment according to the results of genotyping or phenotyping testing to detect DPD deficiency will provide critical information on the best strategy to identify DPD deficiency.

Published

2020

30. Dextromethorphan and memantine after ketamine analgesia: a randomized control trial.

Author

Martin E, Sorel M, Morel V, Marcaillou F, Picard P, Delage N, Tiberghien F, Crosmary MC, Najjar M, Colamarino R, Créach C, Lietar B, Brumauld de Montgazon G, Margot-Duclot A, Loriot MA, Narjoz C, Lambert C, Pereira B, and Pickering G

Subjects

Administration, Oral, Adult, Aged, Dextromethorphan administration & dosage, Female, Humans, Infusions, Intravenous, Ketamine administration & dosage, Male, Memantine administration & dosage, Middle Aged, Analgesia, Dextromethorphan therapeutic use, Ketamine therapeutic use, Memantine therapeutic use, Neuralgia drug therapy

Abstract

Purpose: Intravenous ketamine is often prescribed in severe neuropathic pain. Oral N -methyl-D-aspartate receptor (NMDAR) antagonists might prolong pain relief, reducing the frequency of ketamine infusions and hospital admissions. This clinical trial aimed at assessing whether oral dextromethorphan or memantine might prolong pain relief after intravenous ketamine., Patients and Methods: A multicenter randomized controlled clinical trial included 60 patients after ketamine infusion for refractory neuropathic pain. Dextromethorphan (90 mg/day), memantine (20 mg/day) or placebo was given for 12 weeks (n=20 each) after ketamine infusion. The primary endpoint was pain intensity at one month. Secondary endpoints included pain, sleep, anxiety, depression, cognitive function and quality of life evaluations up to 12 weeks., Results: At 1 month, dextromethorphan maintained ketamine pain relief (Numeric Pain Scale: 4.01±1.87 to 4.05±2.61, p =0.53) and diminished pain paroxysms ( p =0.03) while pain intensity increased significantly with memantine and placebo ( p =0.04). At 3 months, pain remained lower than at inclusion ( p =0.001) and was not significantly different in the three groups. Significant benefits were observed on cognitive-affective domains and quality of life for dextromethorphan and memantine ( p <0.05)., Conclusions: Oral dextromethorphan given after ketamine infusion extends pain relief during one month and could help patients to better cope with pain. Future studies should include larger populations stratified on pharmacogenetics screening. Optimization of an oral drug that could extend ketamine antihyperalgesia, with fewer hospital admissions, remains a prime challenge in refractory neuropathic pain., Competing Interests: The authors report no conflicts of interest in this work.

Published

2019

31. Dextromethorphan Analgesia in a Human Experimental Model of Hyperalgesia.

Author

Martin E, Narjoz C, Decleves X, Labat L, Lambert C, Loriot MA, Ducheix G, Dualé C, Pereira B, and Pickering G

Subjects

Cross-Over Studies, Double-Blind Method, Humans, Male, Treatment Outcome, Analgesia methods, Dextromethorphan therapeutic use, Excitatory Amino Acid Antagonists therapeutic use, Hyperalgesia drug therapy, Neuralgia drug therapy

Abstract

Background: Central pain sensitization is often refractory to drug treatment. Dextromethorphan, an N-methyl-D-aspartate receptor antagonist, is antihyperalgesic in preclinical pain models. The hypothesis is that dextromethorphan is also antihyperalgesic in humans., Methods: This randomized, double-blind, placebo-controlled, crossover study explores the antihyperalgesic effect of single and repeated 30-mg dose of oral dextromethorphan in 20 volunteers, using the freeze-injury pain model. This model leads to development of primary and secondary hyperalgesia, which develops away from the site of injury and is associated with central sensitization and activation of N-methyl-D-aspartate receptor in the spinal cord. The primary outcome was antihyperalgesia calculated with the area under the curve of the percentage change in mechanical pain threshold (electronic von Frey) on the area of secondary hyperalgesia. The secondary outcomes were mechanical pain threshold on the area of primary hyperalgesia and cognitive (reaction time) effect., Results: Single 30-mg results are reported. Antihyperalgesia (% · min) is significantly higher on the area of secondary hyperalgesia with dextromethorphan than placebo (median [interquartile range]: 3,029 [746; 6,195] vs. 710 [-3,248; 4,439], P = 0.009, Hedge's g = 0.8, 95% CI [0.1; 1.4]). On primary hyperalgesia area, mechanical pain threshold 2 h after drug intake is significantly higher with dextromethorphan (P = 0.011, Hedge's g = 0.63, 95% CI [0.01; 1.25]). No difference in antinociception is observed after thermal painful stimuli on healthy skin between groups. Reaction time (ms) is shorter with placebo than with dextromethorphan (median [interquartile range]: 21.6 [-37.4; 0.1] vs. -1.2 [-24.3; 15.4], P = 0.015, Hedge's g = 0.75, 95% CI [0.12; 1.39]). Nonserious adverse events occurrence (15%, 3 of 20 volunteers) was similar in both groups., Conclusions: This study shows that low-dose (30-mg) dextromethorphan is antihyperalgesic in humans on the areas of primary and secondary hyperalgesia and reverses peripheral and central neuronal sensitization. Because dextromethorphan had no intrinsic antinociceptive effect in acute pain on healthy skin, N-methyl-D-aspartate receptor may need to be sensitized by pain for dextromethorphan to be effective.

Published

2019

32. Determinants of the interindividual variability in serum cytidine deaminase activity of patients with solid tumours.

Author

Cohen R, Preta LH, Joste V, Curis E, Huillard O, Jouinot A, Narjoz C, Thomas-Schoemann A, Bellesoeur A, Tiako Meyo M, Quilichini J, Desaulle D, Nicolis I, Cessot A, Vidal M, Goldwasser F, Alexandre J, and Blanchet B

Subjects

Aged, Antimetabolites, Antineoplastic adverse effects, Biomarkers, Tumor genetics, Cytidine Deaminase genetics, Deoxycytidine adverse effects, Deoxycytidine therapeutic use, Female, Humans, Inflammation blood, Inflammation enzymology, Male, Malnutrition blood, Malnutrition enzymology, Malnutrition physiopathology, Middle Aged, Neutrophils, Nutritional Status, Pancreatic Neoplasms blood, Pancreatic Neoplasms enzymology, Pharmacogenomic Variants, Polymorphism, Single Nucleotide, Prospective Studies, Gemcitabine, Antimetabolites, Antineoplastic therapeutic use, Biological Variation, Population, Biomarkers, Tumor blood, Cytidine Deaminase blood, Deoxycytidine analogs & derivatives, Drug Monitoring methods, Pancreatic Neoplasms drug therapy

Abstract

Aims: Cytidine deaminase (CDA) activity in cancer patients' serum has been proposed as a predictive biomarker for efficacy and toxicity of nucleoside analogues. However, discrepant results about its predictive value have been reported due to the high interindividual variability in CDA activity. This study aimed at identifying determinants of this interindividual variability., Methods: From December 2014 to November 2015, 183 patients were prospectively included. Serum CDA activity, biological and clinical characteristics as well as five common single nucleotide polymorphisms (SNPs) in the CDA gene (c.-451C > T, c.-92A > G, c.-33&#95;-31delC, c.79A > C, c.435 T > C) were analysed. Associations between clinical characteristics, pharmacogenetic variants and CDA activity were univariately tested. P < 0.1-candidate variables were analysed through a multivariate analysis. The association between CDA activity and toxicity was assessed for the 56 gemcitabine-treated patients. Intraindividual variability in CDA activity was explored in six pancreatic cancer patients treated with gemcitabine., Results: Median CDA activity was 3.97 U mg -1 (range 1.53-15.49 U mg -1 ). A univariate analysis showed that CDA activity was statistically associated with Eastern Cooperative Oncology Group performance status, mild or severe malnutrition, inflammatory syndrome, leucocyte count, neutrophil count, albumin, C-reactive protein and -c.-33&#95;-31delC single nucleotide polymorphism. A multivariate analysis identified that only neutrophil count (P < 0.0001) and severe malnutrition (P = 0.0278) were independently associated with CDA activity. Low CDA activity (<2 U mg -1 ) was not statistically associated with severe gemcitabine-related toxicities (P = 0.16). A decrease in CDA activity was observed during the longitudinal follow-up of six pancreatic cancer patients treated with gemcitabine (P = 0.03)., Conclusions: These results suggest that neutrophil count and malnutrition should be considered for the interpretation of pretherapeutic CDA activity., (© 2018 The British Pharmacological Society.)

Published

2019

33. [Dihydropyrimidine déhydrogenase (DPD) deficiency screening and securing of fluoropyrimidine-based chemotherapies: Update and recommendations of the French GPCO-Unicancer and RNPGx networks].

Author

Loriot MA, Ciccolini J, Thomas F, Barin-Le-Guellec C, Royer B, Milano G, Picard N, Becquemont L, Verstuyft C, Narjoz C, Schmitt A, Bobin-Dubigeon C, Harle A, Paci A, Poinsignon V, Quaranta S, Evrard A, Hennart B, Broly F, Fonrose X, Lafay-Chebassier C, Wozny AS, Masskouri F, Boyer JC, and Etienne-Grimaldi MC

Subjects

Antimetabolites, Antineoplastic administration & dosage, Antimetabolites, Antineoplastic adverse effects, Capecitabine administration & dosage, Capecitabine adverse effects, Dihydropyrimidine Dehydrogenase Deficiency diagnosis, Dihydrouracil Dehydrogenase (NADP) analysis, Dihydrouracil Dehydrogenase (NADP) genetics, Fluorouracil administration & dosage, Fluorouracil adverse effects, France, Humans, Neoplasms drug therapy, Phenotype, Practice Guidelines as Topic, Pyrimidines administration & dosage, Pyrimidines adverse effects, Pyrimidines therapeutic use, Uracil blood, Antimetabolites, Antineoplastic therapeutic use, Capecitabine therapeutic use, Dihydropyrimidine Dehydrogenase Deficiency complications, Fluorouracil therapeutic use

Abstract

Fluoropyrimidines (FU) are still the most prescribed anticancer drugs for the treatment of solid cancers. However, fluoropyrimidines cause severe toxicities in 10 to 40% of patients and toxic deaths in 0.2 to 0.8% of patients, resulting in a real public health problem. The main origin of FU-related toxicities is a deficiency of dihydropyrimidine dehydrogenase (DPD), the rate-limiting enzyme of 5-FU catabolism. DPD deficiency may be identified through pharmacogenetics testing including phenotyping (direct or indirect measurement of enzyme activity) or genotyping (detection of inactivating polymorphisms on the DPYD gene). Approximately 3 to 15% of patients exhibit a partial deficiency and 0.1 to 0.5% a complete DPD deficiency. Currently, there is no regulatory obligation for DPD deficiency screening in patients scheduled to receive a fluoropyrimidine-based chemotherapy. Based on the levels of evidence from the literature data and considering current French practices, the Group of Clinical Pharmacology in Oncology (GPCO)-UNICANCER and the French Network of Pharmacogenetics (RNPGx) recommend the following: (1) to screen DPD deficiency before initiating any chemotherapy containing 5-FU or capecitabine; (2) to perform DPD phenotyping by measuring plasma uracil (U) concentrations (possibly associated with dihydrouracil/U ratio), and DPYD genotyping (variants *2A, *13, p.D949V, HapB3); (3) to reduce the initial FU dose (first cycle) according to DPD status, if needed, and further, to consider increasing the dose at subsequent cycles according to treatment tolerance. In France, 17 public laboratories currently undertake routine screening of DPD deficiency., (Copyright © 2018 Société Française du Cancer. Published by Elsevier Masson SAS. All rights reserved.)

Published

2018

34. [Lynch syndrome and endometrial cancer].

Author

Bats AS, Rossi L, Le Frere-Belda MA, Narjoz C, Cournou C, Gosset M, Ngo C, Delomenie M, Nos C, Blons H, Laurent-Puig P, and Lecuru F

Subjects

Age Factors, Aged, Colorectal Neoplasms, Hereditary Nonpolyposis pathology, Colorectal Neoplasms, Hereditary Nonpolyposis therapy, Endometrial Neoplasms pathology, Endometrial Neoplasms therapy, Female, Humans, Microsatellite Instability, Middle Aged, Mutation, Colorectal Neoplasms, Hereditary Nonpolyposis genetics, DNA Mismatch Repair, Endometrial Neoplasms genetics

Abstract

Lynch syndrome is a hereditary predisposition to many tumors, in the forefront of which endometrial cancer in women. It is related to the mutation of a mismatch repair gene, involved in DNA mismatch repair. This mutation leads to a loss of expression of the corresponding protein, and to genome instability in tumor cells. Cumulative risk at the age of 70 years is over 40 %. Endometrial cancers related to Lynch syndrome are most of the time sentinel (They reveal the predisposition in half of families.) and are characterized by young age at onset (before 60 years) and low body mass index compared with patients presenting sporadic tumors. Pathological tumor characteristics are debated but it seems to be two types of tumors according to age, older patients having standard tumors and younger ones more aggressive pattern. Endometrial cancers related to Lynch syndrome can be synchronous of ovarian cancer. Therapeutic management does not present any particularity. Conservative treatment can be considered more frequently due to young age of patients but has to respect usual guidelines. Prognosis of these tumors is controversial. Gynaecological screening, although its benefit has not been proved, appears crucial in this population, as well as prophylactic surgery, which remains the best prevention., (Copyright © 2017 Société Française du Cancer. Published by Elsevier Masson SAS. All rights reserved.)

Published

2017

35. Roles of APOL1 G1 and G2 variants in sickle cell disease patients: kidney is the main target.

Author

Kormann R, Jannot AS, Narjoz C, Ribeil JA, Manceau S, Delville M, Joste V, Prié D, Pouchot J, Thervet E, Courbebaisse M, and Arlet JB

Subjects

Adult, Black or African American, Apolipoprotein L1, Female, Glomerular Filtration Rate, Glutathione S-Transferase pi genetics, Glutathione Transferase genetics, Heme Oxygenase-1 genetics, Humans, Male, Albuminuria genetics, Albuminuria physiopathology, Anemia, Sickle Cell genetics, Anemia, Sickle Cell physiopathology, Apolipoproteins genetics, Genetic Variation, Heterozygote, Homozygote, Kidney physiopathology, Lipoproteins, HDL genetics

Abstract

In African-American patients with sickle cell disease (SCD), APOL1 G1 and G2 variants are associated with increased risk of sickle cell nephropathy (SCN). To determine the role of APOL1 variants in SCD patients living in Europe, we genotyped 152 SCD patients [aged 30·4 (24·3-36·4) years], mainly of Sub-Saharan African ancestry, for APOL1 G1 and G2 and for variants of four genes with kidney tropism (GSTM1, GSTT1, GSTP1, and HMOX1). Homozygous or double-heterozygous APOL G1 and G2 genotypes were strongly associated with end stage renal disease (P = 0·003) and worse Kidney Disease: Improving Global Outcomes stages (P = 0·001). Further, these genotypes were associated in an age-dependent manner with lower estimated glomerular filtration rate (eGFR, P = 0·008), proteinuria (P = 0·009) and albuminuria (P < 0·001) but not with other SCD complications. Compared to APOL1 G1/wild type (WT), the APOL1 G2/WT genotype was associated with a lower eGFR (P = 0·04) in an age-dependent manner, suggesting that the G2/WT patients are likely to have worse kidney prognosis. Other genes variants analysed were not associated with SCN or other SCD complications. Our data indicate that APOL1 screening should be considered for the management of SCD patients, including those of non-African-American origin, as those with homozygous or double heterozygous variants are clearly at higher risk of SCN., (© 2017 John Wiley & Sons Ltd.)

Published

2017

36. Pegylated liposomal doxorubicin (Caelyx®) interference with the spectrophotometric Jaffe method for quantitative determination of creatinine in human plasma.

Author

Blel A, Orven Y, Pallet N, Chasse JF, Vedie B, Loriot MA, Paul JL, and Narjoz C

Subjects

Aged, Artifacts, Doxorubicin analogs & derivatives, Female, Humans, Polyethylene Glycols, Retrospective Studies, Creatinine blood, Spectrophotometry methods

Published

2017

37. Interindividual variability in dabigatran and rivaroxaban exposure: contribution of ABCB1 genetic polymorphisms and interaction with clarithromycin.

Author

Gouin-Thibault I, Delavenne X, Blanchard A, Siguret V, Salem JE, Narjoz C, Gaussem P, Beaune P, Funck-Brentano C, Azizi M, Mismetti P, and Loriot MA

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, ATP Binding Cassette Transporter, Subfamily B, Member 1 antagonists & inhibitors, Adolescent, Adult, Alleles, Area Under Curve, Cytochrome P-450 CYP3A, Cytochrome P-450 CYP3A Inhibitors pharmacokinetics, Genotype, Heterozygote, Homozygote, Humans, Male, Middle Aged, Mutation, Young Adult, Clarithromycin pharmacokinetics, Dabigatran pharmacokinetics, Polymorphism, Genetic, Rivaroxaban pharmacokinetics

Abstract

Essentials Rivaroxaban and dabigatran are substrates of the P-glycoprotein (P-gp) encoded by the ABCB1 gene. We tested the effect of ABCB1 polymorphisms and of a P-gp inhibitor on both drugs' pharmacokinetics. The ABCB1 genotype was not a clinically relevant determinant of both drugs' pharmacokinetics. Administration of P-gp inhibitors with dabigatran or rivaroxaban should be exercised with caution., Summary: Background The direct oral anticoagulants (DOACs) dabigatran and rivaroxaban are both substrates of the P-glycoprotein (P-gp) transporter, encoded by the ABCB1 gene. Rivaroxaban is metabolized by cytochrome P450 A4 (CYP3A4). Interindividual variability in DOAC exposure and frequent P-gp-associated drug-drug interactions have been described in patients. Objective To assess the influence of ABCB1 polymorphisms on the pharmacokinetics of dabigatran and rivaroxaban, associated or not with clarithromycin, a P-gp and CYP3A4 inhibitor. Methods Sixty healthy male volunteers, selected according to ABCB1 genotype (20 homozygous mutated, 20 heterozygous mutated, and 20 wild-type for haplotype 2677-3435), were included in this randomized, two-center, crossover study. All received sequentially a single dose of dabigatran etexilate (300 mg) and rivaroxaban (40 mg) associated or not with clarithromycin. Peak plasma concentration and area under the curve (AUC) were compared across the three ABCB1 genotypes. The effect of clarithromycin on dabigatran or rivaroxaban pharmacokinetics was assessed. Results Interindividual coefficients of variation for AUC were 77% for dabigatran and 51% for rivaroxaban. ABCB1 genotype did not significantly affect drug pharmacokinetics: AUC ratios between mutant-allele carriers and wild-type volunteers were 1.27 (95% confidence interval [CI] 0.84-1.92) and 1.20 (95% CI 0.96-1.51) for dabigatran and rivaroxaban, respectively. Clarithromycin coadministration led to a two-fold increase in both drugs' AUC, irrespective of ABCB1 genotype: ratios of geometric means were 2.0 (95% CI 1.15-3.60) and 1.94 (95% CI 1.42-2.63) for dabigatran and rivaroxaban, respectively. Conclusions ABCB1 genotype is not a significant determinant of interindividual variability in dabigatran and rivaroxaban pharmacokinetics. The levels of one drug did not predict the levels of the other. Coadministration of a P-gp/CYP3A4 inhibitor with dabigatran or rivaroxaban may warrant caution in patients at risk of overexposure., (© 2016 International Society on Thrombosis and Haemostasis.)

Published

2017

38. Relation between plasma trough concentration of abiraterone and prostate-specific antigen response in metastatic castration-resistant prostate cancer patients.

Author

Carton E, Noe G, Huillard O, Golmard L, Giroux J, Cessot A, Saidu NE, Peyromaure M, Zerbib M, Narjoz C, Guibourdenche J, Thomas A, Vidal M, Goldwasser F, Blanchet B, and Alexandre J

Subjects

Aged, Aged, 80 and over, Androgen Antagonists blood, Androgen Antagonists therapeutic use, Androstenes blood, Androstenes therapeutic use, Disease-Free Survival, Humans, Kaplan-Meier Estimate, Logistic Models, Male, Prospective Studies, Prostatic Neoplasms, Castration-Resistant blood, Androgen Antagonists pharmacokinetics, Androstenes pharmacokinetics, Prostate-Specific Antigen blood, Prostatic Neoplasms, Castration-Resistant drug therapy

Abstract

Background: Abiraterone (ABI) is a major oral agent for the treatment of metastatic castration-resistant prostate cancer (mCRPC) patients but its systemic exposure is subject to a large inter-individual variability. We aimed to explore the relationship between ABI trough plasma concentration and prostate-specific antigen (PSA) response in mCRPC patients and to identify the critical determinants for its activity., Patients and Methods: This is a monocentric prospective observational study in mCRPC patients treated with ABI. The plasmatic concentration of ABI at steady state was measured using liquid chromatography with fluorescence detection. The primary objective was to study the relationship between mean ABI plasma exposure (ABI C min ) and 3-month PSA response., Results: From 2012 to 2016, 61 mCRPC patients were eligible for pharmacokinetic/pharmacodynamic assessment. Thirty-eight patients experienced PSA response (62%, [confidence interval {CI} 95% 50-78]). In univariate analysis, ABI C min was 1.5-fold higher in responders: 12.0 ng/mL (CI 95% 9.4-15.6) versus 8.0 ng/mL (CI 95% 5.8-11.6; P = 0.0015). In multivariate analysis, only ABI C min was independently associated with PSA response (odds ratio = 1.12 [CI 95% 1.01-1.25], P = 0.004). By receiver operating characteristic analysis, the optimal threshold for ABI C min was 8.4 ng/mL. Progression-free survival (PFS) was significantly higher in patients with ABI C min above 8.4 ng/mL (hazard ratio 0.55, [CI 95% 0.31-0.99], 12.2 [CI 95% 9.2-19.5] versus 7.4 [CI 95% 5.5-14.7] months otherwise, P = 0.044)., Conclusions: We showed that ABI trough concentration correlates with PSA response and PFS. Moreover, we could determine a cut-off value of plasmatic concentration for PSA response. Altogether, ABI concentration monitoring appears as a new approach to improve clinical outcome in mCPRC patients., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2017

39. Safety and pharmacokinetics of the CIME combination of drugs and their metabolites after a single oral dosing in healthy volunteers.

Author

Lenuzza N, Duval X, Nicolas G, Thévenot E, Job S, Videau O, Narjoz C, Loriot MA, Beaune P, Becquemont L, Mentré F, Funck-Brentano C, Alavoine L, Arnaud P, Delaforge M, and Bénech H

Subjects

Administration, Oral, Adult, Cytochrome P-450 Enzyme System metabolism, Drug-Related Side Effects and Adverse Reactions etiology, Drug-Related Side Effects and Adverse Reactions metabolism, Female, Healthy Volunteers, Humans, Male, Pilot Projects, Young Adult, Drug Interactions, Pharmaceutical Preparations metabolism

Abstract

This phase I, pilot clinical study was designed to evaluate the safety and the pharmacokinetic (PK) profiles of the CIME (Metabolic Identity Card) combination of ten drugs, with a view to its use as a phenotyping cocktail. Ten healthy Caucasian subjects were orally dosed with the CIME combination (caffeine-CYP1A2, repaglinide-CYP2C8, tolbutamide-CYP2C9, omeprazole-CYP2C19, dextromethorphan-CYP2D6, midazolam-CYP3A, acetaminophen-UGT1A1, 6&9 and 2B15, digoxin-P-gp, rosuvastatin-OATP1B1&3 and memantine-active renal transport). Blood was collected over 3 days and on day 7. CIME probes and relevant metabolites were assayed by LC-MS/MS and PK parameters were calculated. Main results were: (1) good safety with reversible mild or moderate adverse effects, (2) an analytical method able to quantify simultaneously the 10 probes and the major metabolites, (3) calculation of PK parameters for all probes in general agreed with published values, and (4) identification of the low CYP2D6 metabolizer. This pilot study showed that the CIME combination was well tolerated and that its pharmacokinetics could be accurately measured in healthy volunteers. This combination can now confidently be checked for sensitivity and specificity and for lack of interaction to be validated as a phenotyping cocktail.

Published

2016

40. UGT1A1 genotype and irinotecan therapy: general review and implementation in routine practice.

Author

Etienne-Grimaldi MC, Boyer JC, Thomas F, Quaranta S, Picard N, Loriot MA, Narjoz C, Poncet D, Gagnieu MC, Ged C, Broly F, Le Morvan V, Bouquié R, Gaub MP, Philibert L, Ghiringhelli F, and Le Guellec C

Abstract

Irinotecan is a major drug in the treatment of advanced colorectal cancer. Its active form is the SN38 metabolite, which is cleared by the biliary route after glucuronidation by uridine diphosphate-glucuronosyltransferase 1A1 (UGT1A1). UGT1A1 activity exhibits a wide intersubject variability, in part related to UGT1A1 gene polymorphisms. The present review on the impact of the deficient UGT1A1*28 variant on irinotecan efficacy and toxicity was produced by a French joint workgroup comprising the Group of Clinical Onco-pharmacology (GPCO-Unicancer) and the National Pharmacogenetics Network (RNPGx). It clearly emerges that for irinotecan doses at least equal to 180 mg/m(2) , patients homozygous for the UGT1A1*28 allele are at increased risk of developing hematological and/or digestive toxicities. Irinotecan dose reduction is thus recommended in homozygous *28/*28 patients. In addition, this personalized medicine strategy aims to secure high-dose irinotecan administration (≥240 mg/m(2) ) that have proven to be safe in homozygous *1/*1 patients only. The clinical relevance of this test is discussed in terms of treatment efficacy improvement, as increasing the irinotecan dose appears to be safe in patients not bearing a deficient allele. Best execution practices, cost-effectiveness, and result interpretation are discussed with the aim of facilitating the implementation of this analysis in clinical practice. The existence of networks of laboratories performing this test in routine hospital treatment, as in France, offers the prospect of widespread screening, thus guaranteeing equal access to safe treatment and optimized therapy for patients receiving irinotecan-based therapy in advanced colorectal cancer., (© 2015 Société Française de Pharmacologie et de Thérapeutique.)

Published

2015

41. Role of the lean body mass and of pharmacogenetic variants on the pharmacokinetics and pharmacodynamics of sunitinib in cancer patients.

Author

Narjoz C, Cessot A, Thomas-Schoemann A, Golmard JL, Huillard O, Boudou-Rouquette P, Behouche A, Taieb F, Durand JP, Dauphin A, Coriat R, Vidal M, Tod M, Alexandre J, Loriot MA, Goldwasser F, and Blanchet B

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, ATP Binding Cassette Transporter, Subfamily G, Member 2, Aged, Constitutive Androstane Receptor, Cytochrome P-450 CYP3A genetics, Female, Humans, Male, Middle Aged, Neoplasms genetics, Neoplasms metabolism, Pharmacogenetics, Polymorphism, Genetic, Receptors, Steroid genetics, Sunitinib, Treatment Outcome, ATP-Binding Cassette Transporters genetics, Angiogenesis Inhibitors adverse effects, Angiogenesis Inhibitors pharmacokinetics, Angiogenesis Inhibitors therapeutic use, Body Weight, Indoles adverse effects, Indoles blood, Indoles pharmacokinetics, Indoles therapeutic use, Neoplasm Proteins genetics, Neoplasms drug therapy, Protein Kinase Inhibitors adverse effects, Protein Kinase Inhibitors pharmacokinetics, Protein Kinase Inhibitors therapeutic use, Pyrroles adverse effects, Pyrroles blood, Pyrroles pharmacokinetics, Pyrroles therapeutic use

Abstract

Introduction: Sunitinib is a multikinase inhibitor active in various cancers types including renal cancers and endocrine tumors. The study analyzed the influence of the lean body mass (LBM) and of pharmacogenetic variants on the exposure to sunitinib and its active metabolite, SU12662, and on sunitinib toxicity and clinical activity., Materials and Methods: Exposure to sunitinib and SU12662 was assessed on days 10 and 21 during the first treatment cycle. Acute toxicity was graded using the NCI 4.0 CTCAE ver. 4.0. The LBM and 14 common single nucleotide polymorphisms in the CYP3A4/3A5, NR1I2, NR1I3, ABCB1, and ABCG2 genes were analyzed according to the drug exposure at day 10. Determinants (including sunitinib exposure and pharmacogenetic variants) for toxicities were assessed, as well as the relationship between drug exposure and survival in renal cancer patients., Results: Ninety-two patients (60 % with renal cancer) were assessable for pharmacokinetics, toxicity and survival, and 66 for genetic analysis. The LBM (p < 0.0001) and a polymorphism in the ABCG2 transporter (421C>A) (p = 0.014) were two independent parameters accounting for the variability of composite (sunitinib + SU12662) exposure. Advanced age (OR = 1.47 [1.01-2.15], p = 0.048) and high sunitinib exposure (OR = 1.16 [1.05-1.28], p = 0.005) were independently associated with any grade ≥ 3 acute toxicity, and high SU12662 exposure was associated with grade ≥ 2 thrombocytopenia (OR = 1.27 [1.03-1.57], p = 0.028). A high composite area under the curve (AUC) >1,973 ng/mL∙h at day 21 was associated with a doubled survival (35.2 vs 16.7 months; log-rank p = 0.0051) in renal cancer patients., Conclusions: This study indicates that LBM and drug monitoring may be helpful in the management of sunitinib-treated patients.

Published

2015

42. Microsatellite instability analysis in uterine cavity washings to detect endometrial cancer in Lynch syndrome.

Author

Bats AS, Blons H, Narjoz C, Le Frere-Belda MA, Laurent-Puig P, and Lecuru F

Subjects

Colorectal Neoplasms, Hereditary Nonpolyposis complications, Colorectal Neoplasms, Hereditary Nonpolyposis pathology, Endometrial Neoplasms etiology, Feasibility Studies, Female, Follow-Up Studies, Humans, Middle Aged, Prognosis, Uterine Neoplasms etiology, Uterus pathology, Colorectal Neoplasms, Hereditary Nonpolyposis surgery, Endometrial Neoplasms diagnosis, Hysterectomy adverse effects, Microsatellite Instability, Therapeutic Irrigation, Uterine Neoplasms diagnosis

Abstract

Aim: To assess the feasibility of Microsatellite Instability (MSI) analysis in uterine cavity washings for detecting endometrial cancer in Lynch syndrome., Materials and Methods: This was a proof-of-concept study in Lynch syndrome patients, scheduled for hysterectomy. At the beginning of surgical procedure, uterine cavity washings were performed, and sent for MSI analysis. Pathological examination of the uterus was associated with mismatch repair protein expression and MSI analysis., Results: Nine patients were included in the study. Uterine cavity washings were feasible and interpretable in all cases. Final histological report identified 2 endometrial cancers and 7 benign specimens. There was no atypical hyperplasia. Sensitivity, specificity, positive predictive value, and negative predictive value of MSI analysis in uterine washings reached 100% in all cases. Concordance of MSI presence or absence was absolute between uterine washings and final histology., Conclusion: MSI analysis in uterine cavity washings may be a promising screening tool for Lynch syndrome-associated endometrial cancer diagnosis., (Copyright© 2014 International Institute of Anticancer Research (Dr. John G. Delinassios), All rights reserved.)

Published

2014

43. Important role of CYP2J2 in protein kinase inhibitor degradation: a possible role in intratumor drug disposition and resistance.

Author

Narjoz C, Favre A, McMullen J, Kiehl P, Montemurro M, Figg WD, Beaune P, de Waziers I, and Rochat B

Subjects

Benzamides metabolism, Carcinoma, Hepatocellular genetics, Cell Line, Tumor, Cytochrome P-450 CYP1A1 genetics, Cytochrome P-450 CYP1B1 genetics, Cytochrome P-450 CYP2J2, Cytochrome P-450 CYP3A genetics, Cytochrome P-450 Enzyme System genetics, Dasatinib, Hep G2 Cells, Humans, Imatinib Mesylate, Indoles metabolism, Liver Neoplasms genetics, Niacinamide analogs & derivatives, Niacinamide metabolism, Phenylurea Compounds metabolism, Piperazines metabolism, Pyrimidines metabolism, Pyrroles metabolism, Reverse Transcriptase Polymerase Chain Reaction, Sorafenib, Sunitinib, Thiazoles metabolism, Cytochrome P-450 Enzyme System metabolism, Protein Kinase Inhibitors metabolism

Abstract

We have investigated in vitro the metabolic capability of 3 extrahepatic cytochromes P-450, CYP1A1, 1B1 and 2J2, known to be over-expressed in various tumors, to biotransform 5 tyrosine kinase inhibitors (TKI): dasatinib, imatinib, nilotinib, sorafenib and sunitinib. Moreover, mRNA expression of CYP1A1, 1B1, 2J2 and 3A4 in 6 hepatocellular and 14 renal cell carcinoma tumor tissues and their surrounding healthy tissues, was determined. Our results show that CYP1A1, 1B1 and especially 2J2 can rapidly biotransform the studied TKIs with a metabolic efficiency similar to that of CYP3A4. The mRNA expression of CYP1A1, 1B1, 2J2 and 3A4 in tumor biopsies has shown i) the strong variability of CYP expression and ii) distinct outliers showing high expression levels (esp. CYP2J2) that are compatible with high intratumoral CYP activity and tumor-specific TKI degradation. CYP2J2 inhibition could be a novel clinical strategy to specifically increase the intratumoral rather than plasma TKI levels, improving TKI efficacy and extending the duration before relapse. Such an approach would be akin to beta-lactamase inhibition, a classical strategy to avoid antibiotic degradation and resistance.

Published

2014

44. APOL1 polymorphisms and development of CKD in an identical twin donor and recipient pair.

Author

Kofman T, Audard V, Narjoz C, Gribouval O, Matignon M, Leibler C, Desvaux D, Lang P, and Grimbert P

Subjects

Apolipoprotein L1, Apolipoproteins metabolism, Biopsy, Follow-Up Studies, Genetic Predisposition to Disease, Genotype, Humans, Kidney pathology, Lipoproteins, HDL metabolism, Male, Renal Insufficiency, Chronic metabolism, Renal Insufficiency, Chronic surgery, Young Adult, Apolipoproteins genetics, Diseases in Twins, Kidney Transplantation adverse effects, Lipoproteins, HDL genetics, Living Donors, Polymorphism, Genetic, Renal Insufficiency, Chronic genetics, Twins, Monozygotic genetics

Abstract

We report an occurrence of progressive loss of transplant function and ultimately transplant failure after living related kidney transplantation involving monozygotic twin brothers of Afro-Caribbean origin who were both heterozygous for the G1 and G2 kidney disease risk alleles in the APOL1 gene, which encodes apolipoprotein L-I. A 21-year-old man with end-stage kidney disease of unknown cause received a kidney from his brother, who was confirmed as a monozygotic twin by microsatellite analysis. Thirty months after transplantation, the patient presented with proteinuria and decreased estimated glomerular filtration rate; a biopsy of the transplant showed typical focal segmental glomerulosclerosis lesions. He received steroid therapy, but progressed to kidney failure 5 years later. The twin brother had normal kidney function without proteinuria at the time of transplantation; however, 7 years later, he was found to have decreased estimated glomerular filtration rate (40mL/min/1.73m(2)) and proteinuria (protein excretion of 2.5g/d). APOL1 genotyping revealed that both donor and recipient were heterozygous for the G1 and G2 alleles. This case is in stark contrast to the expected course of kidney transplantation in identical twins and suggests a role for APOL1 polymorphisms in both the donor and recipient., (Copyright © 2014 National Kidney Foundation, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2014

45. Interindividual variability in TPMT enzyme activity: 10 years of experience with thiopurine pharmacogenetics and therapeutic drug monitoring.

Author

Chouchana L, Narjoz C, Roche D, Golmard JL, Pineau B, Chatellier G, Beaune P, and Loriot MA

Subjects

Adult, Azathioprine administration & dosage, Databases, Factual, Drug Monitoring methods, Female, Genotype, Guanine Nucleotides administration & dosage, Guanine Nucleotides metabolism, Humans, Male, Middle Aged, Pharmacogenetics methods, Phenotype, Retrospective Studies, Thioguanine metabolism, Thioinosine administration & dosage, Thioinosine analogs & derivatives, Thioinosine metabolism, Thionucleotides administration & dosage, Thionucleotides metabolism, Young Adult, Individuality, Methyltransferases genetics, Methyltransferases metabolism, Thioguanine administration & dosage

Abstract

Background & Aims: TPMT activity and metabolite determination (6-thioguanine nucleotides [6-TGN] and 6-methylmercaptopurine nucleotides [6-MMPN]) remain controversial during thiopurine management. This study assessed associations between patient characteristics and TPMT activity, and their impact on metabolite levels., Patients & Methods: A retrospective review of the laboratory database from a French university hospital identified 7360 patients referred for TPMT phenotype/genotype determination, and/or for 6-TGN/6-MMPN monitoring., Results: Four TPMT phenotypes were identified according to TPMT activity distribution: low, intermediate, normal/high and very high. Based on 6775 assays, 6-TGN concentrations were 1.6-fold higher in TPMT-deficient patients compared with TPMT-normal patients. Azathioprine dose and TPMT genotype were significant predictors of metabolite levels. Furthermore, 6-MMPN and 6-MMPN: 6-TGN ratios were, respectively, 1.6- and 2.2-fold higher in females than in males, despite similar TPMT, 6-TGN and azathioprine doses. An unfavorable ratio (≥20) was associated with a slightly higher TPMT activity., Conclusion: These results illustrate the usefulness of pharmacogenomics and metabolite measurement to improve the identification of noncompliance and patients at high risk for toxicity or therapeutic resistance. Original submitted 13 November 2013; Revision submitted 30 January 2014.

Published

2014

46. A case of 5-FU-related severe toxicity associated with the p.Y186C DPYD variant.

Author

Zaanan A, Dumont LM, Loriot MA, Taieb J, and Narjoz C

Subjects

Female, Humans, Male, Black or African American genetics, Antimetabolites, Antineoplastic therapeutic use, Dihydrouracil Dehydrogenase (NADP) genetics, Fluorouracil therapeutic use, Neoplasms drug therapy

Published

2014

47. Microsatellite instability analysis for the screening of synchronous endometrial and ovarian cancer in Lynch syndrome.

Author

Bats AS, Roussel H, Narjoz C, Le Frere-Belda MA, Chamming's F, Blons H, Laurent-Puig P, and Lecuru F

Subjects

Adaptor Proteins, Signal Transducing genetics, Adult, DNA Mismatch Repair, Endometrial Neoplasms complications, Endometrial Neoplasms surgery, Female, Humans, MutL Protein Homolog 1, Nuclear Proteins genetics, Ovarian Neoplasms complications, Ovarian Neoplasms surgery, Colorectal Neoplasms, Hereditary Nonpolyposis complications, Endometrial Neoplasms diagnosis, Genetic Testing methods, Microsatellite Instability, Ovarian Neoplasms diagnosis

Abstract

We report on a case of synchronous endometrial and ovarian cancer in a patient with Lynch syndrome. An endometrial biopsy performed during routine screening revealed microsatellite instability (MSI) and loss of expression of human mutL homolog-1 (MLH1) and postmeiotic segregation increased-2 (PMS2) in a setting of complex hyperplasia. Whereas gynaecological screening including clinical examination, pelvic ultrasound, and endometrial biopsy, has not proven its benefit, our case report points out the place of MSI analysis and immunohistochemical investigation of mismatch repair protein expression in endometrial samples during gynaecological screening.

Published

2013

48. Collapsing glomerulopathy associated lupus in a black female with homozygous APOL1 mutation.

Author

Kofman T, Narjoz C, Raimbourg Q, Loriot MA, Karras A, Roland M, Hill G, Jacquot C, Nochy D, and Thervet E

Subjects

Apolipoprotein L1, Biopsy, Female, Fluorescent Antibody Technique, Genetic Predisposition to Disease, Humans, Immunosuppressive Agents therapeutic use, Lupus Erythematosus, Systemic ethnology, Lupus Erythematosus, Systemic pathology, Lupus Erythematosus, Systemic therapy, Lupus Nephritis ethnology, Lupus Nephritis pathology, Lupus Nephritis therapy, Phenotype, Plasma Exchange, Predictive Value of Tests, Renal Dialysis, Risk Factors, Treatment Outcome, Young Adult, Black or African American genetics, Apolipoproteins genetics, Homozygote, Kidney Glomerulus pathology, Lipoproteins, HDL genetics, Lupus Erythematosus, Systemic genetics, Lupus Nephritis genetics, Mutation

Abstract

Collapsing glomerulopathy (CG), characterized by collapse of the glomerular capillary loops onto the mesangial stalks is rarely associated to systemic lupus erythematosus (SLE). Recently a genetic predisposition to HIV associated nephropathy (HIVAN) has been shown in Afro-Americans: MYH9 polymorhism in 2008 and then APOL1 variants (G1 and G2 alleles) in 2010 were shown to be strongly associated with HIVAN. We describe here for the first time the association of CG in a young Afro-American female with SLE having a homozygous mutation of APOL1. The clinical history, laboratory findings and immunofluorescence all confirmed a diagnosis of SLE. However, studies for factors associated with collapsing glomerulopathy in other situations were consistently negative. As this Afro-American patient developed a CG, we performed genotyping of APOL1. It was found that she is homozygotic for the G2 allele of APOL1. Despite.

Published

2012

49. TPMT status determination: the simplest is the most effective?

Author

Chouchana L, Narjoz C, and Loriot MA

Subjects

Humans, Azathioprine pharmacokinetics, Genotype, Immunosuppressive Agents pharmacokinetics, Inflammatory Bowel Diseases drug therapy, Mercaptopurine pharmacokinetics, Methyltransferases genetics, Phenotype

Published

2012

50. Early sorafenib-induced toxicity is associated with drug exposure and UGTIA9 genetic polymorphism in patients with solid tumors: a preliminary study.

Author

Boudou-Rouquette P, Narjoz C, Golmard JL, Thomas-Schoemann A, Mir O, Taieb F, Durand JP, Coriat R, Dauphin A, Vidal M, Tod M, Loriot MA, Goldwasser F, and Blanchet B

Subjects

Aged, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Area Under Curve, Diarrhea chemically induced, Female, Genotype, Humans, Hypertension chemically induced, Male, Middle Aged, Neoplasms enzymology, Neoplasms metabolism, Niacinamide adverse effects, Niacinamide pharmacokinetics, Niacinamide pharmacology, Niacinamide therapeutic use, Phenylurea Compounds pharmacokinetics, Phenylurea Compounds pharmacology, Phenylurea Compounds therapeutic use, Risk Factors, Skin drug effects, Sorafenib, UDP-Glucuronosyltransferase 1A9, Antineoplastic Agents adverse effects, Glucuronosyltransferase genetics, Neoplasms drug therapy, Neoplasms genetics, Niacinamide analogs & derivatives, Phenylurea Compounds adverse effects, Polymorphism, Single Nucleotide

Abstract

Background: Identifying predictive biomarkers of drug response is of key importance to improve therapy management and drug selection in cancer therapy. To date, the influence of drug exposure and pharmacogenetic variants on sorafenib-induced toxicity remains poorly documented. The aim of this pharmacokinetic/pharmacodynamic (PK/PD) study was to investigate the relationship between early toxicity and drug exposure or pharmacogenetic variants in unselected adult outpatients treated with single-agent sorafenib for advanced solid tumors., Methods: Toxicity was recorded in 54 patients on days 15 and 30 after treatment initiation and sorafenib exposure was assessed in 51 patients. The influence of polymorphisms in CYP3A5, UGT1A9, ABCB1 and ABCG2 was examined in relation to sorafenib exposure and toxicity. Clinical characteristics, drug exposure and pharmacogenetic variants were tested univariately for association with toxicities. Candidate variables with p<0.1 were analyzed in a multivariate analysis., Results: Gender was the sole parameter independently associated with sorafenib exposure (p = 0.0008). Multivariate analysis showed that increased cumulated sorafenib (AUC(cum)) was independently associated with any grade ≥ 3 toxicity (p = 0.037); UGT1A9 polymorphism (rs17868320) with grade ≥ 2 diarrhea (p = 0.015) and female gender with grade ≥ 2 hand-foot skin reaction (p = 0.018). Using ROC curve, the threshold AUC(cum) value of 3,161 mg/L.h was associated with the highest risk to develop any grade ≥ 3 toxicity (p = 0.018)., Conclusion: In this preliminary study, increased cumulated drug exposure and UGT1A9 polymorphism (rs17868320) identified patients at high risk for early sorafenib-induced severe toxicity. Further PK/PD studies on larger population are warranted to confirm these preliminary results.

Published

2012