Your search keyword '"L Chene"' showing total 7 results

1. 1295P Prognostic impact of baseline tumor size (BTS) on survival outcomes in patients (pts) with untreated advanced non-small cell lung cancer (NSCLC), PD-L1 ≥50%, treated with pembrolizumab alone

Author

R. Affi, Jaafar Bennouna, T. Perennec, Charlotte Greilsamer, T. Goronflot, T. Chatelier, E. Pons-Tostivint, M. Bureau, and A-L. Chene

Subjects

Oncology, medicine.medical_specialty, Tumor size, biology, business.industry, non-small cell lung cancer (NSCLC), Hematology, Pembrolizumab, medicine.disease, Internal medicine, PD-L1, medicine, biology.protein, In patient, business

Published

2021

2. Timing of combined antiretroviral treatment initiation in male and female migrants living with HIV in Western Europe

Author

Monge, S. Jarrín, I. Pantazis, N. Mocroft, A. Sabin, C.A. Touloumi, G. van Sighem, A. Abgrall, S. Dray-Spira, R. Spire, B. Castagna, A. Mussini, C. Zangerle, R. Hessamfar, M. Anderson, J. Hamouda, O. Ehren, K. Obel, N. Kirk, O. de Monteynard, L.A. Antinori, A. Girardi, E. Saracino, A. Calmy, A. de Wit, S. Wittkop, L. Bucher, H.C. Montoliu, A. Raben, D. Prins, M. Meyer, L. Chene, G. Burns, F. Del Amo, J. The Migrant Health Working Group for the Collaboration of Observational HIV Epidemiological Research in Europe (COHERE) in EuroCoord

Subjects

virus diseases

Abstract

Background: We evaluate differences in timing of cART (combined antiretroviral treatment) initiation by geographical origin in male and female HIV-positive patients in the Collaboration of Observational HIV Epidemiological Research Europe, a large European Collaboration of HIV Cohorts. Methods: We included individuals recruited in Western Europe between January 1997 and March 2013, with known geographical origin and at least 1 CD4þ cell count measurement while cART-naive. Timing of cART was assessed through modified time-to-event methods, in which a scale of CD4þ cell counts was used instead of time, with cART being the outcome. We estimated the median CD4þ cell count at cART initiation (estimated CD4þ levels at which the probability of having started cART is 50%) using Kaplan-Meier and adjusted hazard ratios of cART initiation using Cox regression. Results: Of 151 674 individuals, 110 592 (72.9%) were men. Median (95% confidence interval) CD4þ cell count falls far below 250 cells/ml in all groups and was lowest in sub-Saharan African [SSA: 161 (158-167)], Caribbean men [161 (150-174)] and in Asian women [Asian Continent and Oceania: 185 (165-197)]. Among men, the adjusted probability of cART initiation was lower in migrants compared with natives, but differences depended on initial CD4þ cell count. For example, in the group with more than 500 CD4þ at recruitment, they were 45% (36-53%), 30% (17-40%) and 25% (19-30%) lower for Caribbean, Eastern European and SSA men, respectively. In women, no meaningful differences were observed between natives and most migrant groups. However, SSA women had a 31% (24-38%) higher probability of cART initiation when recruited at a CD4þ more than 500 cells/ml and 9% (4-14%) lower when recruited at CD4þ less than 100 cells/ml. Conclusion: Most migrant men initiate cART at lower CD4þ cell count than natives, whereas this does not hold for migrant women. Copyright © 2017 Wolters Kluwer Health, Inc. All rights reserved.

Published

2017

3. Mortality in migrants living with HIV in western Europe (1997-2013): a collaborative cohort study

Author

Monge, S. Jarrin, I. Mocroft, A. Sabin, C. A. Touloumi, G. van Sighem, A. Abgrall, S. Dray-Spira, R. Spire, B. and Castagna, A. Mussini, C. Zangerle, R. Hessamfar, M. and Anderson, J. Hamouda, O. Ehren, K. Obel, N. Kirk, O. and de Monteynard, L. A. Antinori, A. Girardi, E. Saracino, A. and Calmy, A. De Wit, S. Wittkop, L. Bucher, H. C. and Montoliu, A. Raben, D. Prins, M. Meyer, L. Chene, G. and Burns, F. Del Amo, J. COHERE EuroCoord

Abstract

Background Many migrants face adverse socioeconomic conditions and barriers to health services that can impair timely HIV diagnosis and access to life-saving treatments. We aimed to assess the differences in overall mortality by geographical origin in HIV-positive men and women using data from COHERE, a large European collaboration of HIV cohorts from 1997 to 2013. Methods In this observational cohort study, we included HIV-positive, antiretroviral-naive people accessing care in western Europe from COHERE. Individuals were eligible if enrolled in a cohort that collected information on geographical origin or ethnic origin from Jan 1, 1997, to March 19, 2013, aged 18-75 years, they had available information about sex, they were not infected perinatally or after the receipt of clotting factor concentrates, and were naive to combination antiretroviral therapy at cohort entry. Migrants’ origins were grouped into seven regions: western Europe and similar countries (Australia, Canada, New Zealand, and the USA); eastern Europe; North Africa and the Middle East; sub-Saharan Africa; Latin America; the Caribbean; and Asia and the rest of Oceania (excluding Australia and New Zealand). Crude and adjusted mortality rate ratios were calculated by use of Poisson regression stratified by sex, comparing each group with the native population. Multiple imputation with chained equations was used to account for missing values. Findings Between Oct 25, 1979, and March 19, 2013, we recruited 279 659 individuals to the COHERE collaboration in EuroCoord. Of these 123 344 men and 45 877 women met the inclusion criteria. Our data suggested effect modification by transmission route (p(interaction) = 0.12 for men; p (interaction) = 0.002 for women). No significant difference in mortality was identified by geographical origin in men who have sex with men. In heterosexual populations, most migrant men had mortality lower than or equal to that of native men, whereas no group of migrant women had mortality lower than that in native women. High mortality was identified in heterosexual men from Latin America (rate ratio [RR] 1.46, 95% CI 1.00-2.12, p= 0.049) and heterosexual women from the Caribbean (1.48, 1.29-1.70, p< 0.0001). Compared with that in the native population, mortality in injecting drug users was similar or low for all migrant groups. Interpretation Characteristics of and risks faced by migrant populations with HIV differ for men and women and for populations infected heterosexually, by sex between men, or by injecting drug use. Further research is needed to understand how inequalities are generated and maintained for the groups with higher mortality identified in this study.

Published

2015

4. A primary malarial infection is composed of a very wide range of genetically diverse but related parasites

Author

L Chene, Jintana Patarapotikul, T Chongsuphajaisiddhi, C Gentil, P Daubersies, G Langsley, Druilhe P, and Mellouk S

Subjects

Plasmodium falciparum, Drug Resistance, Polymerase Chain Reaction, Insect bites and stings, law.invention, Antimalarials, law, parasitic diseases, Genetic variation, Genotype, medicine, Animals, Humans, Malaria, Falciparum, Primary isolate, Polymerase chain reaction, Genetics, Cloning, Quinine, biology, Genetic Variation, Insect Bites and Stings, Chloroquine, General Medicine, Thailand, medicine.disease, biology.organism_classification, Virology, Clone Cells, Mefloquine, Culicidae, Phenotype, Parasitology, Africa, Biomarkers, Polymorphism, Restriction Fragment Length, Research Article

Abstract

To address the question of how many distinct parasites are injected when a mosquito bites, we have characterized isolates resulting most probably from a single sporozoite inoculum. We describe the direct and immediate cloning on hepatocyte feeder layers of a Thai and an African Plasmodium falciparum primary isolate and the characterization of 67 independent clones by four techniques totaling nine different markers. This led to three main conclusions: (a) both the phenotypic and genotypic markers revealed an unexpectedly large degree of diversity within the clones from a single isolate; (b) the clones are nonetheless genetically related; and (c) a single mosquito inoculum would most likely be sufficient to generate considerable isolate complexity in the absence of repeated exposure. This diversity, which has been greatly underestimated in previous studies, does not bode well for the development of successful malaria control means.

Published

1998

5. Rebetron® therapy of chronic hepatitis C patients who were non-responsive to or relapsed on interferon monotherapy-predicting relapse

Author

Brenda L. Chene, Douglas R. LaBrecque, Mary Jeanne Perino Phillips, Dawn Schrock, Robert Juhl, Edward C. Adler, Laura Ippolito, Carlo H. Tamburro, Michael D. Voigt, Warren N. Schmidt, Anthony Martin, and Donna Brashear

Subjects

medicine.medical_specialty, Hepatology, Chronic hepatitis, business.industry, Interferon, Internal medicine, Gastroenterology, Medicine, business, medicine.drug

Published

2000

6. Identification of a muropeptide precursor transporter from gut microbiota and its role in preventing intestinal inflammation.

Author

Liuu S, Nepelska M, Pfister H, Gamelas Magalhaes J, Chevalier G, Strozzi F, Billerey C, Maresca M, Nicoletti C, Di Pasquale E, Pechard C, Bardouillet L, Girardin SE, Boneca IG, Doré J, Blottière HM, Bonny C, Chene L, and Cultrone A

Subjects

Humans, Mice, Animals, Peptidoglycan metabolism, Intestines pathology, Inflammation metabolism, Membrane Transport Proteins metabolism, Anti-Inflammatory Agents metabolism, Dextran Sulfate, Disease Models, Animal, Colon metabolism, Mice, Inbred C57BL, Gastrointestinal Microbiome, Colitis metabolism

Abstract

The gut microbiota is a considerable source of biologically active compounds that can promote intestinal homeostasis and improve immune responses. Here, we used large expression libraries of cloned metagenomic DNA to identify compounds able to sustain an anti-inflammatory reaction on host cells. Starting with a screen for NF-κB activation, we have identified overlapping clones harbouring a heterodimeric ATP-binding cassette (ABC)-transporter from a Firmicutes. Extensive purification of the clone's supernatant demonstrates that the ABC-transporter allows for the efficient extracellular accumulation of three muropeptide precursor, with anti-inflammatory properties. They induce IL-10 secretion from human monocyte-derived dendritic cells and proved effective in reducing AIEC LF82 epithelial damage and IL-8 secretion in human intestinal resections. In addition, treatment with supernatants containing the muropeptide precursor reduces body weight loss and improves histological parameters in Dextran Sulfate Sodium (DSS)-treated mice. Until now, the source of peptidoglycan fragments was shown to come from the natural turnover of the peptidoglycan layer by endogenous peptidoglycan hydrolases. This is a report showing an ABC-transporter as a natural source of secreted muropeptide precursor and as an indirect player in epithelial barrier strengthening. The mechanism described here might represent an important component of the host immune homeostasis., Competing Interests: Competing interests statement:M.N., J.D., H.M.B., A.C., and C. Bonny are the inventors of a patent application protecting the heterodimeric transporter (WO 2021/​148661). The other authors have no conflicts of interest to declare aside from the fact that several of the authors are employees of private companies.

Published

2023

7. A primary malarial infection is composed of a very wide range of genetically diverse but related parasites.

Author

Druilhe P, Daubersies P, Patarapotikul J, Gentil C, Chene L, Chongsuphajaisiddhi T, Mellouk S, and Langsley G

Subjects

Africa, Animals, Antimalarials pharmacology, Biomarkers, Chloroquine pharmacology, Clone Cells, Culicidae parasitology, Drug Resistance, Humans, Insect Bites and Stings, Mefloquine pharmacology, Parasitology methods, Phenotype, Plasmodium falciparum isolation & purification, Polymerase Chain Reaction, Quinine pharmacology, Thailand, Genetic Variation, Malaria, Falciparum parasitology, Plasmodium falciparum genetics, Polymorphism, Restriction Fragment Length

Abstract

To address the question of how many distinct parasites are injected when a mosquito bites, we have characterized isolates resulting most probably from a single sporozoite inoculum. We describe the direct and immediate cloning on hepatocyte feeder layers of a Thai and an African Plasmodium falciparum primary isolate and the characterization of 67 independent clones by four techniques totaling nine different markers. This led to three main conclusions: (a) both the phenotypic and genotypic markers revealed an unexpectedly large degree of diversity within the clones from a single isolate; (b) the clones are nonetheless genetically related; and (c) a single mosquito inoculum would most likely be sufficient to generate considerable isolate complexity in the absence of repeated exposure. This diversity, which has been greatly underestimated in previous studies, does not bode well for the development of successful malaria control means.

Published

1998