Your search keyword '"Cedrick Wallet"' showing total 6 results

1. Correlation between blood telomere length and CD4+ CD8+ T-cell subsets changes 96 weeks after initiation of antiretroviral therapy in HIV-1-positive individuals.

Author

Mathieu Chalouni, Javier Rodriguez-Centeno, Assia Samri, Julian Blanco, Natalia Stella-Ascariz, Cedrick Wallet, Hernando Knobel, David Zucman, Belen Alejos Ferreras, Brigitte Autran, Rodolphe Thiebaut, François Raffi, Jose Ramon Arribas, and NEAT 001/ANRS 143 Trial Study Group

Subjects

Medicine, Science

Abstract

In 31 participants who started first-line antiretroviral therapy in the NEAT 001/ANRS 143 clinical trial, we found after 96 weeks a statistically significant increase in blood telomere length (TL) of 0.04 (T/S Ratio) (p = 0.03). This increase was positively correlated with both the change in the percentage of CD4+ T-cells and with the decrease of CD38+ molecules on Central Memory CD8+ and negatively correlated with the change in the percentage of CD4+ Effector Memory cells. Increase in TL could be an expression of immune reconstitution and the associated decrease in immune activation. We acknowledge for the low statistical power due to the small sample size and the potential for false positive results due to multiple testing. Hence, further studies are needed to confirm these observations.

Published

2020

2. Body composition and adipokines changes after initial treatment with darunavir-ritonavir plus either raltegravir or tenofovir disoproxil fumarate-emtricitabine: A substudy of the NEAT001/ANRS143 randomised trial.

Author

Jose I Bernardino, Amanda Mocroft, Cedrick Wallet, Stéphane de Wit, Christine Katlama, Peter Reiss, Patrick W Mallon, Laura Richert, Jean-Michel Molina, Hernando Knobel, Philippe Morlat, Abdel Babiker, Anton Pozniac, Francois Raffi, Jose R Arribas, and NEAT001/ANRS143 Trial Study Group

Subjects

Medicine, Science

Abstract

BackgroundComparison of changes in body composition, adipokines and inflammatory markers after initial therapy with a nucleos(t)ide reverse transcriptase inhibitor (N(t)RTI)- sparing or containing regimen are scarce.DesignRandomised Clinical Trial.MethodsThis is the body composition substudy of NEAT 001/ANRS 143, a randomised trial comparing darunavir/ritonavir (DRV/r) plus either raltegravir (RAL) or tenofovir disoproxil fumarate/emtricitabine (TDF/FTC) in 805 ART naïve HIV-infected adults. The primary endpoint was percentage change in limb fat at week 96. Secondary endpoints were associations among these changes and metabolic markers (IL-6, insulin, leptin, adiponectin, FGF-23).Results126 subjects (61 DRV/r + RAL and 65 DRV/r + TDF/FTC) were included. The rate of change in BMI between groups for RAL versus TDF/FTC at week 96 was 1.5% per 48-week period (p = 0.015). The rate of change in limb fat mass, trunk fat mass, total body fat and total lean mass was for RAL versus TDF/FTC at week 96 was 2.5% (p = 0.38), 7.3% ((p = 0.021), 4.9% (p = 0.061) and 1.3% (p = 0.12) respectively. Baseline insulin and leptin levels were correlated with baseline limb fat and trunk fat mass [r = 0.31 (p = 0.0043)/r = 0.28 (p = 0.0011) for limb fat, and r = 0.63 (pConclusionsAfter week 96 a N(t)RTI sparing regimen of DRV/r + RAL produced a numerically greater percentage increase in body composition variables with only change in trunk fat mass and BMI being significant.

Published

2019

3. Worry and ruminative brooding: associations with cognitive and physical health in older adults

Author

Rachel M. Morse, Freya Koutsoubelis, Tim Whitfield, Harriet Demnitz-King, Valentin Ourry, Josh Stott, Anne Chocat, Eglantine Ferrand Devouge, Zuzana Walker, Olga Klimecki, Fabienne Collette, Gael Chetelat, Julie Gonneaud, Geraldine Poisnel, Natalie L. Marchant, for the Medit-Ageing Research Group, Florence Allais, Claire André, Eider Arenaza-Urquijo, Romain Bachelet, Sebastian Baez Lugo, Thorsten Barnhofer, Maelle Botton, Nina Coll-Padros, Robin De Flores, Vincent De La Sayette, Marion Delarue, Stéphanie Egret, Hélène Espérou, Eric Frison, Karine Goldet, Idir Hamdidouche, Marc Heidmann, Agathe Joret Philippe, Elizabeth Kuhn, Renaud La Joie, Brigitte Landeau, Gwendoline Le Du, Valérie Lefranc, Maria Leon, Dix Meiberth, Florence Mezenge, Inés Moulinet, Cassandre Palix, Léo Paly, Anne Quillard, Géraldine Rauchs, Stéphane Rehel, Florence Requier, Leslie Reyrolle, Laura Richert, Ana Salinero, Eric Salmon, Raquel Sanchez, Lena Sannemann, Ann-Katrin Schild, Marco Schlosser, Clémence Tomadesso, Edelweiss Touron, Denis Vivien, Patrik Vuilleumier, and Cédrick Wallet

Subjects

worry, rumination, cognition, physical health, perseverative cognition, repetitive negative thinking, Psychology, BF1-990

Abstract

IntroductionMental health conditions are associated with cognition and physical function in older adults. We examined whether worry and ruminative brooding, key symptoms of certain mental health conditions, are related to subjective and/or objective measures of cognitive and physical (cardiovascular) health.MethodsWe used baseline data from 282 participants from the SCD-Well and Age-Well trials (178 female; agemean = 71.1 years). We measured worry and ruminative brooding using the Penn State Worry Questionnaire and the Ruminative Response Scale-brooding subscale. We assessed subjective physical health using the WHOQOL-Bref physical subscale, and objective physical health via blood pressure and modified versions of the Framingham Risk Score and Charlson Comorbidity Index. With subjective and objective cognition, we utilized the Cognitive Difficulties Scale and a global composite (modified Preclinical Alzheimer’s Cognitive Composite, PACC5, with the Wechsler Adult Intelligence Scale-IV, category fluency, Mattis Dementia Rating Scale-2, and either the California Verbal Learning Test or the Rey Auditory Verbal Learning Test). We conducted linear regressions, adjusted for education, age, sex and cohort.ResultsWorry and ruminative brooding were negatively associated with subjective physical health (worry: β = −0.245, 95%CI −0.357 to −0.133, p

Published

2024

4. Effect of HIV infection and antiretroviral therapy initiation on genome-wide DNA methylation patternsResearch in context

Author

Andrés Esteban-Cantos, Javier Rodríguez-Centeno, Juan C. Silla, Pilar Barruz, Fátima Sánchez-Cabo, Gabriel Saiz-Medrano, Julián Nevado, Beatriz Mena-Garay, María Jiménez-González, Rosa de Miguel, Jose I. Bernardino, Rocío Montejano, Julen Cadiñanos, Cristina Marcelo, Lucía Gutiérrez-García, Patricia Martínez-Martín, Cédrick Wallet, François Raffi, Berta Rodés, and José R. Arribas

Subjects

HIV infection, Epigenetics, Genome-wide DNA methylation, Antiretroviral therapy, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: Previous epigenome-wide association studies have shown that HIV infection can disrupt the host DNA methylation landscape. However, it remains unclear how antiretroviral therapy (ART) affects the HIV-induced epigenetic modifications. Methods: 184 individuals with HIV from the NEAT001/ANRS143 clinical trial (with pre-ART and post-ART samples [96 weeks of follow-up]) and 44 age-and-sex matched individuals without HIV were included. We compared genome-wide DNA methylation profiles in whole blood between groups adjusting for age, sex, batch effects, and DNA methylation-based estimates of leucocyte composition. Findings: We identified 430 differentially methylated positions (DMPs) between HIV+ pre-ART individuals and HIV-uninfected controls. In participants with HIV, ART initiation modified the DNA methylation levels at 845 CpG positions and restored 49.3% of the changes found between HIV+ pre-ART and HIV-uninfected individuals. We only found 15 DMPs when comparing DNA methylation profiles between HIV+ post-ART individuals and participants without HIV. The Gene Ontology enrichment analysis of DMPs associated with untreated HIV infection revealed an enrichment in biological processes regulating the immune system and antiviral responses. In participants with untreated HIV infection, DNA methylation levels at top HIV-related DMPs were associated with CD4/CD8 ratios and viral loads. Changes in DNA methylation levels after ART initiation were weakly correlated with changes in CD4+ cell counts and the CD4/CD8 ratio. Interpretation: Control of HIV viraemia after 96 weeks of ART initiation partly restores the host DNA methylation changes that occurred before antiretroviral treatment of HIV infection. Funding: NEAT-ID Foundation and Instituto de Salud Carlos III, co-funded by European Union.

Published

2023

5. Molecular profiling of advanced soft-tissue sarcomas: the MULTISARC randomized trial

Author

Antoine Italiano, Derek Dinart, Isabelle Soubeyran, Carine Bellera, Hélène Espérou, Christelle Delmas, Noémie Mercier, Sabrina Albert, Ludivine Poignie, Anne Boland, Aurélien Bourdon, Damien Geneste, Quentin Cavaille, Yec’han Laizet, Emmanuel Khalifa, Céline Auzanneau, Barbara Squiban, Nathalène Truffaux, Robert Olaso, Zuzana Gerber, Cédrick Wallet, Antoine Bénard, Jean-Yves Blay, Pierre Laurent-Puig, Jean-François Deleuze, Carlo Lucchesi, Simone Mathoulin-Pelissier, and the MULTISARC study group

Subjects

Next generation sequencing, Soft-tissue sarcomas, Umbrella, Biomarker-driven, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Soft-tissue sarcomas (STS) represent a heterogeneous group of rare tumors including more than 70 different histological subtypes. High throughput molecular analysis (next generation sequencing exome [NGS]) is a unique opportunity to identify driver mutations that can change the usual one-size-fits-all treatment paradigm to a patient-driven therapeutic strategy. The primary objective of the MULTISARC trial is to assess whether NGS can be conducted for a large proportion of metastatic STS participants within a reasonable time, and, secondarily to determine whether a NGS-guided therapeutic strategy improves participant’s outcome. Methods This is a randomized, multicentre, phase II/III trial inspired by the design of umbrella and biomarker-driven trials. The setting plans up to 17 investigational centres across France and the recruitment of 960 participants. Participants aged at least 18 years, with unresectable locally advanced and/or metastatic STS confirmed by the French sarcoma pathological reference network, are randomized according to 1:1 allocation ratio between the experimental arm “NGS” and the standard “No NGS”. NGS will be considered feasible if (i) NGS results are available and interpretable, and (ii) a report of exome sequencing including a clinical recommendation from a multidisciplinary tumor board is provided to investigators within 7 weeks from reception of the samples on the biopathological platform. A feasibility rate of more than 70% is expected (null hypothesis: 70% versus alternative hypothesis: 80%). In terms of care, participants randomized in “No NGS” arm and who fail treatment will be able to switch to the NGS arm at the request of the investigator. Discussion The MULTISARC trial is a prospective study designed to provide high-level evidence to support the implementation of NGS in routine clinical practice for advanced STS participants, on a large scale. Trial registration clinicaltrial.gov NCT03784014 .

Published

2021

6. COL05-01 RAL + DRV/r est non inférieur à TDF/FTC + DRV/r en traitement initial antirétroviral : essai NEAT001/ANRS143

Author

Juliette Saillard, Cedrick Wallet, F. Raffi, L. Niedbalski, P. Perré, C. Allavena, and Christine Katlama

Subjects

Infectious Diseases

Abstract

Introduction – objectifs NEAT001/ANRS143 est un essai randomise de non-inferiorite, sans insu, comparant DRV/r associe a RAL ou TDF/FTC en 1re ligne de traitement antiretroviral chez les adultes VIH+. Materiels et methodes Le critere de jugement principal etait le delai jusqu’a l’echec virologique (changement de traitement pour baisse de charge virale (CV) Resultats 805 patients (RAL n = 401, TDF/FTC n = 404, 88 % d’hommes) ont ete inclus, avec en mediane : âge 38 ans, CV 4,77 log10 c/ml, CD4 333/mm3, suivi de 123 semaines. A S96 (RAL vs TDF/FTC), la proportion d’echec etait de 17,4 % vs 13,7 % (difference : 3,7 % ; IC95 % : -1,1 ; 8,6 %) ; celle d’echec ou d’arret du traitement initial etait de 22,8 % vs 19,5 % (difference : 3,3 % ; IC95 % : -1,9 ; 8,4 %) ; le taux (pour 100 patient-annees) d’evenements indesirables (EI) severes etait de 10,2 vs 8,3 (p = 0,17), d’EI de grade 3-4 de 9,6 vs 7,4 (p = 0,16), d’EI entrainant le changement de traitement de 4,2 vs 4,2 (p = 0,84). La CV etait Conclusion Le schema d’epargne d’INTI associant RAL et DRV/r est non inferieur a TDF/FTC + DRV/r en termes de reponse virologique et clinique a S96 et peut representer une alternative en 1re ligne de traitement ARV.

Published

2014