Your search keyword '"Corthesy P"' showing total 44 results

1. The mediating role of kynurenine pathway metabolites on the relationship between inflammation and muscle mass in oldest-old men.

Author

Hetherington-Rauth, Megan, Johnson, Eileen, Migliavacca, Eugenia, Langsetmo, Lisa, Hepple, Russell T, Ryan, Terence E, Ferrucci, Luigi, Breuillé, Denis, Corthesy, John, Lane, Nancy E, Feige, Jérôme N, Napoli, Nicola, Tramontana, Flavia, Orwoll, Eric S, and Cawthon, Peggy M

Subjects

C-reactive protein, D3-creatine, biomarkers, sarcopenia, Clinical Sciences, Gerontology, Biomedical and clinical sciences, Health sciences

Abstract

Tryptophan (TRP) metabolites along the kynurenine (KYN) pathway (KP) have been found to influence muscle. Pro-inflammatory cytokines are known to stimulate the degradation of TRP down the KP. Given that both inflammation and KP metabolites have been connected with loss of muscle, we assessed the potential mediating role of KP metabolites on inflammation and muscle mass in older men. 505 men (85.0±4.2yrs) from the Osteoporotic Fractures in Men cohort study with measured D3-creatine dilution (D3Cr) muscle mass, KP metabolites, and inflammation markers (C-reactive protein (CRP), alpha-1-acid glycoprotein (AGP) and a subsample (n=305) with interleukin (IL-6, IL-1β, IL-17A) and tumor necrosis factor-α (TNF-α)) were included in the analysis. KP metabolites and inflammatory markers were measured using liquid chromatography-tandem mass spectrometry and immunoassays, respectively. 23-92% of the inverse relationship between inflammatory markers and D3Cr muscle mass was mediated by KP metabolites (indirect effect p0.05). KP metabolites, particularly higher ratios of KYN/TRP, 3-HK/XA, 3-HK/3-HAA, QA/3-HAA and a lower ratio of NAM/QA, mediated the relationship between inflammation and low muscle mass. Our preliminary cross-sectional data suggest that interventions to alter D3Cr muscle mass may focus on KP metabolites rather than inflammation per se.

Published

2024

2. Effect of an enteral amino acid blend on muscle and gut functionality in critically ill patients: a proof-of-concept randomized controlled trial

Author

Nicholas Heming, Robert Carlier, Helene Prigent, Ahmed Mekki, Camille Jousset, Frederic Lofaso, Xavier Ambrosi, Rania Bounab, Virginie Maxime, Arnaud Mansart, Pascal Crenn, Pierre Moine, Fabien Foltzer, Bernard Cuenoud, Tobias Konz, John Corthesy, Maurice Beaumont, Mickaël Hartweg, Claudia Roessle, Jean-Charles Preiser, Denis Breuillé, and Djillali Annane

Subjects

Sepsis, Critical illness, Protein balance, Intensive care unit, Nutrition, Medical emergencies. Critical care. Intensive care. First aid, RC86-88.9

Abstract

Abstract Background A defining feature of prolonged critical illness is muscle wasting, leading to impaired recovery. Supplementation with a tailored blend of amino acids may bolster the innate gut defence, promote intestinal mucosa repair and limit muscle loss. Methods This was a monocentric, randomized, double-blind, placebo-controlled study that included patients with sepsis or acute respiratory distress syndrome. Patients received a specific combination of five amino acids or placebo mixed with enteral feeding for 21 days. Markers of renal function, gut barrier structure and functionality were collected at baseline and 1, 2, 3 and 8 weeks after randomization. Muscle structure and function were assessed through MRI measurements of the anterior quadriceps volume and by twitch airway pressure. Data were compared between groups relative to the baseline. Results Thirty-five critically ill patients were randomized. The amino acid blend did not impair urine output, blood creatinine levels or creatinine clearance. Plasma citrulline levels increased significantly along the treatment period in the amino acid group (difference in means [95% CI] 5.86 [1.72; 10.00] nmol/mL P = 0.007). Alanine aminotransferase and alkaline phosphatase concentrations were lower in the amino acid group than in the placebo group at one week (ratio of means 0.5 [0.29; 0.86] (P = 0.015) and 0.73 [0.57; 0.94] (P = 0.015), respectively). Twitch airway pressure and volume of the anterior quadriceps were greater in the amino acid group than in the placebo group 3 weeks after randomization (difference in means 10.6 [0.99; 20.20] cmH20 (P = 0.035) and 3.12 [0.5; 5.73] cm3/kg (P = 0.022), respectively). Conclusions Amino acid supplementation increased plasma citrulline levels, reduced alanine aminotransferase and alkaline phosphatase levels, and improved twitch airway pressure and anterior quadriceps volume. Trial registration ClinicalTrials.gov, NCT02968836. Registered November 21, 2016.

Published

2022

3. Corrigendum: A MALDI-TOF MS library for rapid identification of human commensal gut bacteria from the class Clostridia

Author

Paul Tetteh Asare, Chi-Hsien Lee, Vera Hürlimann, Youzheng Teo, Aline Cuénod, Nermin Akduman, Cordula Gekeler, Afrizal Afrizal, Myriam Corthesy, Claire Kohout, Vincent Thomas, Tomas de Wouters, Gilbert Greub, Thomas Clavel, Eric G. Pamer, Adrian Egli, Lisa Maier, and Pascale Vonaesch

Subjects

human gut microbiota, Clostridia, MALDI-TOF MS, commensal bacteria, anaerobic, bacterial identification, Microbiology, QR1-502

Published

2023

4. Effect of an enteral amino acid blend on muscle and gut functionality in critically ill patients: a proof-of-concept randomized controlled trial

Author

Heming, Nicholas, Carlier, Robert, Prigent, Helene, Mekki, Ahmed, Jousset, Camille, Lofaso, Frederic, Ambrosi, Xavier, Bounab, Rania, Maxime, Virginie, Mansart, Arnaud, Crenn, Pascal, Moine, Pierre, Foltzer, Fabien, Cuenoud, Bernard, Konz, Tobias, Corthesy, John, Beaumont, Maurice, Hartweg, Mickaël, Roessle, Claudia, Preiser, Jean-Charles, Breuillé, Denis, and Annane, Djillali

Published

2022

5. A MALDI-TOF MS library for rapid identification of human commensal gut bacteria from the class Clostridia

Author

Paul Tetteh Asare, Chi-Hsien Lee, Vera Hürlimann, Youzheng Teo, Aline Cuénod, Nermin Akduman, Cordula Gekeler, Afrizal Afrizal, Myriam Corthesy, Claire Kohout, Vincent Thomas, Tomas de Wouters, Gilbert Greub, Thomas Clavel, Eric G. Pamer, Adrian Egli, Lisa Maier, and Pascale Vonaesch

Subjects

human gut microbiota, Clostridia, MALDI-TOF MS, commensal bacteria, anaerobic, bacterial identification, Microbiology, QR1-502

Abstract

IntroductionMicrobial isolates from culture can be identified using 16S or whole-genome sequencing which generates substantial costs and requires time and expertise. Protein fingerprinting via Matrix-assisted Laser Desorption Ionization–time of flight mass spectrometry (MALDI-TOF MS) is widely used for rapid bacterial identification in routine diagnostics but shows a poor performance and resolution on commensal bacteria due to currently limited database entries. The aim of this study was to develop a MALDI-TOF MS plugin database (CLOSTRI-TOF) allowing for rapid identification of non-pathogenic human commensal gastrointestinal bacteria.MethodsWe constructed a database containing mass spectral profiles (MSP) from 142 bacterial strains representing 47 species and 21 genera within the class Clostridia. Each strain-specific MSP was constructed using >20 raw spectra measured on a microflex Biotyper system (Bruker-Daltonics) from two independent cultures.ResultsFor validation, we used 58 sequence-confirmed strains and the CLOSTRI-TOF database successfully identified 98 and 93% of the strains, respectively, in two independent laboratories. Next, we applied the database to 326 isolates from stool of healthy Swiss volunteers and identified 264 (82%) of all isolates (compared to 170 (52.1%) with the Bruker-Daltonics library alone), thus classifying 60% of the formerly unknown isolates.DiscussionWe describe a new open-source MSP database for fast and accurate identification of the Clostridia class from the human gut microbiota. CLOSTRI-TOF expands the number of species which can be rapidly identified by MALDI-TOF MS.

Published

2023

6. Association of amino acid metabolites with osteoporosis, a metabolomic approach: Bushehr elderly health program

Author

Panahi, Nekoo, Fahimfar, Noushin, Roshani, Shahin, Arjmand, Babak, Gharibzadeh, Safoora, Shafiee, Gita, Migliavacca, Eugenia, Breuille, Denis, Feige, Jerome N., Grzywinski, Yohan, Corthesy, John, Razi, Farideh, Heshmat, Ramin, Nabipour, Iraj, Farzadfar, Farshad, Soltani, Akbar, Larijani, Bagher, and Ostovar, Afshin

Published

2022

7. A Randomized Controlled Clinical Trial in Healthy Older Adults to Determine Efficacy of Glycine and N-Acetylcysteine Supplementation on Glutathione Redox Status and Oxidative Damage

Author

Giulia Lizzo, Eugenia Migliavacca, Daniela Lamers, Adrien Frézal, John Corthesy, Gerard Vinyes-Parès, Nabil Bosco, Leonidas G. Karagounis, Ulrike Hövelmann, Tim Heise, Maximilian von Eynatten, and Philipp Gut

Subjects

glycine, n-acetylcysteine, glutathione, total cysteine, cardiometabolic diseases, healthy aging, Geriatrics, RC952-954.6

Abstract

Glycine and cysteine are non-essential amino acids that are required to generate glutathione, an intracellular tripeptide that neutralizes reactive oxygen species and prevents tissue damage. During aging glutathione demand is thought to increase, but whether additional dietary intake of glycine and cysteine contributes towards the generation of glutathione in healthy older adults is not well understood. We investigated supplementation with glycine and n-acetylcysteine (GlyNAC) at three different daily doses for 2 weeks (low dose: 2.4 g, medium dose: 4.8 g, or high dose: 7.2 g/day, 1:1 ratio) in a randomized, controlled clinical trial in 114 healthy volunteers. Despite representing a cohort of healthy older adults (age mean = 65 years), we found significantly higher baseline levels of markers of oxidative stress, including that of malondialdehyde (MDA, 0.158 vs. 0.136 µmol/L, p < 0.0001), total cysteine (Cysteine-T, 314.8 vs. 276 µM, p < 0.0001), oxidized glutathione (GSSG, 174.5 vs. 132.3 µmol/L, p < 0.0001), and a lower ratio of reduced to oxidized glutathione (GSH-F:GSSG) (11.78 vs. 15.26, p = 0.0018) compared to a young reference group (age mean = 31.7 years, n = 20). GlyNAC supplementation was safe and well tolerated by the subjects, but did not increase levels of GSH-F:GSSG (end of study, placebo = 12.49 vs. 7.2 g = 12.65, p-value = 0.739) or that of total glutathione (GSH-T) (end of study, placebo = 903.5 vs. 7.2 g = 959.6 mg/L, p-value = 0.278), the primary endpoint of the study. Post-hoc analyses revealed that a subset of subjects characterized by high oxidative stress (above the median for MDA) and low baseline GSH-T status (below the median), who received the medium and high doses of GlyNAC, presented increased glutathione generation (end of study, placebo = 819.7 vs. 4.8g/7.2 g = 905.4 mg/L, p-value = 0.016). In summary GlyNAC supplementation is safe, well tolerated, and may increase glutathione levels in older adults with high glutathione demand.Clinical Trial Registration: https://clinicaltrials.gov/ct2/show/NCT05041179, NCT05041179.

Published

2022

8. Secretory IgA in complex with Lactobacillus rhamnosus potentiates mucosal dendritic cell-mediated Treg cell differentiation via TLR regulatory proteins, RALDH2 and secretion of IL-10 and TGF-β

Author

Mikulic, Josip, Longet, Stéphanie, Favre, Laurent, Benyacoub, Jalil, and Corthesy, Blaise

Published

2017

9. Dietary tryptophan-rich protein hydrolysate can acutely impact physiological and psychological measures of mood and stress in healthy adults

Author

Zahar, Sélima, Schneider, Nora, Makwana, Aidan, Chapman, Stephen, Corthesy, John, Amico, Maïlis, and Hudry, Julie

Abstract

ABSTRACTBackgroundTryptophan is the precursor to the mood regulating neurotransmitter serotonin. Its brain bioavailability from food can be dependent on the dietary source. Egg protein hydrolysate (EPH), a dietary supplement rich in tryptophan, has previously shown to acutely impact cognition, mood and stress benefits at 2 g dose. No data exist on the acute effects of lower doses in a food matrix.MethodsThis exploratory study tested the acute effects of low-doses EPH (0.5, 1 g) in a food matrix on cognition, mood and stress. The study employed a double-blinded randomized controlled parallel design in 45 participants with three arms. The effects of the interventions were measured after a multi-task cognitive stressor on blood biomarkers, self-reported mood states, performances of attention, autonomic parameters and, emotional reactivity responses from electroencephalographic recording.ResultsAs compared to the reference, the 1 g EPH dose increased tryptophan bioavailability from baseline, and, both doses improved heart rate variability parameters related to parasympathetic activation while showing differences in the late neural response to negative versus neutral emotions. Post-hoc analyses indicated a gender difference in the baseline tryptophan bioavailability and further examination suggested the change in mood rating depends on the interaction between gender and change from baseline of tryptophan bioavailability.ConclusionsOverall, this study suggests that low levels of tryptophan rich EPH in a food matrix positively impact mood or stress in acute settings and adds to the body of evidence linking tryptophan and dietary sources thereof with these benefits. Confirmatory randomized controlled trials are needed to confirm these findings.Trial registration number:CER-VD N°2019-00218

Published

2023

10. Selection of Human Single Chain Fv Antibody Fragments Binding and Inhibiting Helicobacter pyloriUrease

Author

Houimel, Mehdi, Corthesy-Theulaz, Irène, Fisch, Igor, Wong, Cindy, Corthesy, Blaise, Mach, Jean-Pierre, and Finnern, Ricarda

Abstract

Single chain Fv antibody fragments (scFv) binding to purified Helicobacter pyloriurease were selected from a nonimmune human antibody repertoire displayed on filamentous phage. After three rounds of screening on solid phase urease, 44 clones were found to bind the enzyme and four distinct scFv were identified by sequencing their heavy and light chain variable region genes (VH and VL). Two of the selected human scFv (scFv B4 and scFv D9) inhibited the activity of H. pyloriurease with inhibitory constants (Ki) of 7 and 2 μM,respectively. Their affinity (Kd) for H. pylori urease as determined by surface plasmon resonance ranged from 17 to 42 nM. Both scFv were able to bind to urease present on the surface of living H. pylori organisms as demonstrated by flow cytometry analysis. The binding sites of scFv B4 and D9 were mapped by the use of two random hexapeptide libraries (X6 and CX6C) displayed on filamentous bacteriophage. The selected peptide sequences were shown to inhibit scFv binding to H. pylori urease and thus could be used in a vaccination strategy as epitopes mimicking (mimotopes) the region of urease recognized by these human scFv antibody fragments.

Published

2001

11. La CIF-EA : une approche pertinente pour évaluer l’impact de l’environnement sur la participation des élèves ?

Author

Guerdan, Viviane, Belet, Cécile, Corthesy, Carole, Jaccottet, Antoine, and Gigon, Vincent

Subjects

STUDENT participation, SPECIAL education, TEACHER education, MASTER'S degree, ESTIMATION theory, STATISTICAL hypothesis testing

Abstract

Copyright of ALTER: European Journal of Disability Research, Journal Europeen de Erche sur le Handicap is the property of European Society for Disability Research and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2013

12. Transgenomic Metabolic Interactions in a Mouse Disease Model:  Interactions of Trichinella spiralisInfection with Dietary Lactobacillus paracasei Supplementation

Author

J. Martin, Francois-Pierre, F. Verdu, Elena, Wang, Yulan, Dumas, Marc-Emmanuel, K. S. Yap, Ivan, Cloarec, Olivier, E. Bergonzelli, Gabriela, Corthesy-Theulaz, Irene, Kochhar, Sunil, Holmes, Elaine, C. Lindon, John, M. Collins, Stephen, and K. Nicholson, Jeremy

Abstract

Irritable Bowel Syndrome (IBS) is a common multifactorial intestinal disorder for which the aetiology remains largely undefined. Here, we have used a Trichinella spiralis(T. spiralis)-induced model of post-infective IBS, and the effects of probiotic bacteria on gut dysfunction have been investigated using a metabonomic strategy. A total of 44 mice were divided into four groups:  an uninfected control group and three T. spiralis-infected groups, one as infected control and the two other groups subsequently treated with either Lactobacillus paracasei(L. paracasei) NCC2461 in spent culture medium (SCM) or with L. paracasei-free SCM. Plasma, jejunal wall and longitudinal myenteric muscle samples were collected at day 21 post-infection. An NMR-based metabonomic approach characterized that the plasma metabolic profile of T. spiralis-infected mice showed an increased energy metabolism (lactate, citrate, alanine), fat mobilization (acetoacetate, 3-D-hydroxybutyrate, lipoproteins) and a disruption of amino acid metabolism due to increased protein breakdown, which were related to the intestinal hypercontractility. Increased levels of taurine, creatine and glycerophosphorylcholine in the jejunal muscles were associated with the muscular hypertrophy and disrupted jejunal functions. L. paracasei treatment normalized the muscular activity and the disturbed energy metabolism as evidenced by decreased glycogenesis and elevated lipid breakdown in comparison with untreated T. spiralis-infected mice. Changes in the levels of plasma metabolites (glutamine, lysine, methionine) that might relate to a modulation of immunological responses were also observed in the presence of the probiotic treatment. The work presented here suggests that probiotics may be beneficial in patients with IBS.

Published

2006

13. Neonatal antibiotic treatment alters gastrointestinal tract developmental gene expression and intestinal barrier transcriptome

Author

Schumann, Alexandra, Nutten, Sophie, Donnicola, Dominique, Comelli, Elena M., Mansourian, Robert, Cherbut, Christine, Corthesy-Theulaz, Irène, and Garcia-Rodenas, Clara

Abstract

The postnatal maturation of the gut, partially modulated by bacterial colonization, ends up in the establishment of an efficient barrier to luminal antigens and bacteria. The use of broad-spectrum antibiotics in pediatric practices alters the gut bacterial colonization and, consequently, may impair the maturation of the gut barrier function. To test this hypothesis, suckling Sprague-Dawley rats received a daily intragastric gavage of antibiotic (Clamoxyl; an amoxicillin-based commercial preparation) or saline solution from postnatal day 7(d7) until d17 or d21. Luminal microbiota composition and global gene expression profile were analyzed on samples from small intestine and colon of each group. The treatment with Clamoxyl resulted in the almost-complete eradication of Lactobacillusin the whole intestine and in a drastic reduction of colonic total aerobic and anaerobic bacteria, in particular Enterobacteriacaeand Enterococcus. The global gene expression analysis revealed that Clamoxyl affects the maturation process of 249 and 149 Affymetrix probe sets in the proximal and distal small intestine, respectively, and 163 probe sets in the colon. The expression of genes coding for Paneth cell products (defensins, matrilysin, and phospholipase A2) was significantly downregulated by the Clamoxyl treatment. A significant downregulation of major histocompatibility complex (MHC) class Ib and II genes, involved in antigen presentation, was also observed. Conversely, mast cell proteases expression was upregulated. These results suggest that early treatment with a large-spectrum antibiotic deeply affects the gut barrier function at the suckling-weaning interface, a period during which the gut is challenged by an array of novel food-borne antigens.

Published

2005

14. Lactobacillus paracasei normalizes muscle hypercontractility in a murine model of postinfective gut dysfunction

Author

Verdu, E.F., Bercik, P., Bergonzelli, G.E., Huang, X.X., Blennerhasset, P., Rochat, F., Fiaux, M., Mansourian, R., Corthesy-Theulaz, I., and Collins, S.M.

Abstract

Background & Aims: The effects of probiotics on gut dysfunction in postinfective irritable bowel syndrome are unknown. We tested whether probiotics influence persistent muscle hypercontractility in mice after recovery from infection with Trichinella spiralis and analyzed the underlying mechanisms. Methods: Mice were gavaged with Lactobacillus paracasei, Lactobacillus johnsonii, Bifidobacterium longum, or Bifidobacterium lactis in spent culture medium from days 10 to 21 after infection. Additional mice received heat-inactivated Lactobacillus paracasei, Lactobacillus paracasei-free spent culture medium, or heat-inactivated Lactobacillus paracasei-free spent culture medium. Lactobacilli enumeration, immunohistochemistry, and cytokine detection (enzyme-linked immunosorbent assay) were performed. Mice were also treated with Lactobacillus paracasei or Lactobacillus paracasei-free spent culture medium from days 18 to 28 after infection. Contractility was measured on days 21 and 28 after infection. Results:Lactobacillus paracasei, but not Lactobacillus johnsonii, Bifidobacterium lactis, or Bifidobacterium longum, attenuated muscle hypercontractility. This was associated with a reduction in the Trichinella spiralis-associated T-helper 2 response and a reduction in transforming growth factor-@b1, cyclooxygenase-2, and prostaglandin E"2 levels in muscle. Attenuation of muscle hypercontractility by Lactobacillus paracasei-free spent culture medium was abolished after heat treatment. Improvement of muscle hypercontractility at day 28 after infection was also observed after the administration ofLactobacillus paracasei or Lactobacillus paracasei-free spent culture medium from day 18 after infection. Conclusions: Probiotics show strain-dependent attenuation of muscle hypercontractility in an animal model of postinfective irritable bowel syndrome. This likely occurs via both a modulation of the immunologic response to infection and a direct effect of Lactobacillus paracasei or a heat-labile metabolite on postinfective muscle hypercontractility. Lactobacillus paracasei may be useful in the treatment of postinfective irritable bowel syndrome.

Published

2004

15. Ex vivo characterization of human CD8+ T subsets with distinct replicative history and partial effector functions

Author

Rufer, Nathalie, Zippelius, Alfred, Batard, Pascal, Pittet, Mikaël J., Kurth, Isabel, Corthesy, Patricia, Cerottini, Jean-Charles, Leyvraz, Serge, Roosnek, Eddy, Nabholz, Markus, and Romero, Pedro

Abstract

After antigenic challenge, naive T lymphocytes enter a program of proliferation and differentiation during the course of which they acquire effector functions and may ultimately become memory cells. In humans, the pathways of effector and memory T-cell differentiation remain poorly defined. Here we describe the properties of 2 CD8+ T-lymphocyte subsets, RA+CCR7–27+28+ and RA+CCR7–27+28–, in human peripheral blood. These cells display phenotypic and functional features that are intermediate between naive and effector T cells. Like naive T lymphocytes, both subsets show relatively long telomeres. However, unlike the naive population, these T cells exhibit reduced levels of T-cell receptor excision circles (TRECs), indicating they have undergone additional rounds of in vivo cell division. Furthermore, we show that they also share effector-type properties. At equivalent in vivo replicative history, the 2 subsets express high levels of Fas/CD95 and CD11a, as well as increasing levels of effector mediators such as granzyme B, perforin, interferon γ, and tumor necrosis factor α. Both display partial ex vivo cytolytic activity and can be found among cytomegalovirus-specific cytolytic T cells. Taken together, our data point to the presence of T cells with intermediate effector-like functions and suggest that these subsets consist of T lymphocytes that are evolving toward a more differentiated effector or effector-memory stage.

Published

2003

16. Ex vivo characterization of human CD8+T subsets with distinct replicative history and partial effector functions

Author

Rufer, Nathalie, Zippelius, Alfred, Batard, Pascal, Pittet, Mikaël J., Kurth, Isabel, Corthesy, Patricia, Cerottini, Jean-Charles, Leyvraz, Serge, Roosnek, Eddy, Nabholz, Markus, and Romero, Pedro

Abstract

After antigenic challenge, naive T lymphocytes enter a program of proliferation and differentiation during the course of which they acquire effector functions and may ultimately become memory cells. In humans, the pathways of effector and memory T-cell differentiation remain poorly defined. Here we describe the properties of 2 CD8+T-lymphocyte subsets, RA+CCR7–27+28+and RA+CCR7–27+28–, in human peripheral blood. These cells display phenotypic and functional features that are intermediate between naive and effector T cells. Like naive T lymphocytes, both subsets show relatively long telomeres. However, unlike the naive population, these T cells exhibit reduced levels of T-cell receptor excision circles (TRECs), indicating they have undergone additional rounds of in vivo cell division. Furthermore, we show that they also share effector-type properties. At equivalent in vivo replicative history, the 2 subsets express high levels of Fas/CD95 and CD11a, as well as increasing levels of effector mediators such as granzyme B, perforin, interferon γ, and tumor necrosis factor α. Both display partial ex vivo cytolytic activity and can be found among cytomegalovirus-specific cytolytic T cells. Taken together, our data point to the presence of T cells with intermediate effector-like functions and suggest that these subsets consist of T lymphocytes that are evolving toward a more differentiated effector or effector-memory stage.

Published

2003

17. Localization of alpha-isoforms of Na(+)-K(+)-ATPase in rat kidney by in situ hybridization

Author

Farman, N., Corthesy-Theulaz, I., Bonvalet, J. P., and Rossier, B. C.

Abstract

The expression of the three alpha-isoforms of Na(+)-K(+)-adenosine triphosphatase (ATPase) was examined in rat brain and rat kidney by Northern blot analysis. All three isoforms were detected in brain tissue while alpha 1-isoform was observed in whole kidney, suggesting that either this isoform was solely expressed in this organ or that alpha 2- and/or alpha 3-isoforms were not detected only because of their restricted distribution among a minority of specialized tubular cells. To distinguish between these two possibilities, in situ hybridization with rat alpha 1-, alpha 2-, and alpha 3-ATPase cRNA was performed on rat kidney sections. Results show that alpha 1-isoform expression largely predominates in the loop of Henle, distal tubule, and cortical collecting tubule. The labeling was drastically reduced by preincubation of sections with RNase. A sense cRNA probe, used as control, did not hybridize. With alpha 2- and alpha 3-probes, the labeling was low and uniformly distributed. In contrast, these two isoforms were clearly expressed in the brain, together with alpha 1. We conclude that only alpha 1-isoform of the Na(+)-K(+)-ATPase is detectable along the rat nephron. Its expression predominates in the tubular segments known to have a high Na(+)-K(+)-ATPase activity.

Published

1991

18. Differential regulation of Na-K-ATPase isoform gene expression by T3 during rat brain development

Author

Corthesy-Theulaz, I., Merillat, A. M., Honegger, P., and Rossier, B. C.

Abstract

A fetal rat telencephalon organotypic cell culture system was found to reproduce the developmental pattern of Na-K-adenosinetriphosphatase (ATPase) gene expression observed in vivo [Am. J. Physiol. 258 (Cell Physiol. 27): C1062-C1069, 1990]. We have used this culture system to study the effects of triiodothyronine (T3; 0.003-30 nM) on mRNA abundance and basal transcription rates of Na-K-ATPase isoforms. Steady-state mRNA levels were low at culture day 6 (corresponding to the day of birth) but distinct for each isoform alpha 3 much greater than beta 1 = beta 2 greater than alpha 2 greater than alpha 1. At culture day 6, T3 did not modify mRNA abundance of any isoform. At culture day 12 (corresponding to day 7 postnatal), T3 increased the mRNA level of alpha 2 (4- to 7-fold), beta 2 (4- to 5-fold), alpha 1 (3- to 6-fold), and beta 1 (1.5-fold), whereas alpha 3 mRNA levels remained unchanged. Interestingly, the basal transcription rate for each isoform differed strikingly (alpha 2 greater than alpha 1 much greater than beta 1 = beta 2 greater than alpha 3) but remained stable throughout 12 days of culture and was not regulated by T3. Thus we observed an inverse relationship between rate of transcription and rate of mRNA accumulation for each alpha-isoform, suggesting that alpha 1- and alpha 2-mRNA are turning over rapidly whereas alpha 3-mRNA is turning over slowly. Our data indicate that one of the mechanisms by which T3 selectively controls Na-K-ATPase gene expression during brain development in vitro occurs at the posttranscriptional level.

Published

1991

19. Immunization of BALB/c mice with Helicobacter urease B induces a T helper 2 response absent in Helicobacter infection

Author

Saldinger, P.F., Porta, N., Launois, P., Louis, J.A., Waanders, G.A., Bouzourene, H., Michetti, P., Blum, A.L., and Corthesy-Theulaz, I.E.

Abstract

Background & Aims: Infection with Helicobacter induces a T helper type 1 response in mice and humans. Mice can be cured or protected from infection with Helicobacter by mucosal immunization with recombinant H. pylori urease B subunit (rUreB). This study characterizes the immune response of infected mice immunized with rUreB. Methods: BALB/c mice were infected with H. felis. Two weeks later, they were orally immunized four times with rUreB and cholera toxin (CT) at weekly intervals. Controls were only infected or sham-immunized with CT. Animals were killed at various times after immunization. Splenic CD4^+ cells were obtained and cultured in vitro with rUreB to evaluate antigen-specific proliferation and induction of interferon gamma and interleukin 4 secretion. Results: All rUreB-immunized mice (n = 8) were cured from infection 3 weeks after the fourth immunization. Immunization induced a proliferative response of splenic CD4^+ cells, a progressive decrease in interferon gamma secretion, and a concomitant increase in interleukin 4 secretion after each immunization. A simultaneous increase in rUreB specific serum immunoglobulin G1 levels was observed in infected/immunized mice. Conclusions: In BALB/c mice, therapeutic mucosal immunization with rUreB induces progressively a Th2 CD4^+ T cell response resulting in the elimination of the pathogen. GASTROENTEROLOGY 1998;115:891-897

Published

1998

20. Polyadenylation of Na(+)-K(+)-ATPase beta 1-subunit during early development of Xenopus laevis

Author

Burgener-Kairuz, P., Corthesy-Theulaz, I., Merillat, A. M., Good, P., Geering, K., and Rossier, B. C.

Abstract

In fully grown Xenopus oocytes, the synthesis of beta-subunits is limiting for the formation of functional Na(+)-K(+)-adenosinetriphosphatase alpha/beta-complexes (Geering, K. FEBS Lett. 285: 189-193, 1991). In the present study, we show that during oocyte growth (from stage I to stage VI) alpha 1-, but not beta 1- or beta 3-isoform, mRNAs accumulate. In addition, beta-mRNAs are apparently sequestered in an untranslated pool in fully grown oocytes (stage VI). From fertilization to morulation, the total pools of alpha 1-, beta 1-, or beta 3-mRNAs vary little. Whereas polyadenylated [poly(A)+] alpha 1- and beta 3-isoform mRNAs did not change significantly, poly(A)+ beta 1-mRNA abundance increased three- to fourfold at morulation, accompanied by a parallel increase in beta 1-protein synthesis. After midblastula transition (i.e., at early gastrula) and during neurulation, poly(A)+ alpha 1- and beta 3-mRNAs accumulated rapidly, whereas poly(A)+ beta 1-mRNA accumulation was delayed by approximately 2 h, beginning only at early neurula. Our results indicate that 1) the abundance of poly(A)+ beta 1-mRNA is rate limiting during embryonic development for the assembly of alpha 1/beta 1-heterodimers, shown to be involved in the vectorial transport of sodium in kidney cells, and 2) the polyadenylation of beta 1-mRNA is a rate-limiting factor during morulation for the synthesis and assembly of new sodium pumps at the time of blastocoel fluid formation. The 3'-untranslated region of beta 1-mRNA (but not of alpha 1-mRNA) expresses cytoplasmic polyadenylation elements (CPEs) with the consensus sequence AXX-AUUUU(A/U)(A/U)(A/U). A role of CPE in the differential polyadenylation of alpha 1- and beta 1-mRNA is proposed.

Published

1994

21. Altered hepatic transport of immunoglobulin A in mice lacking the J chain.

Author

Hendrickson, B A, Conner, D A, Ladd, D J, Kendall, D, Casanova, J E, Corthesy, B, Max, E E, Neutra, M R, Seidman, C E, and Seidman, J G

Abstract

We have created J chain knockout mice to define the physiologic role of the J chain in immunoglobulin synthesis and transport. The J chain is covalently associated with pentameric immunoglobulin (Ig) M and dimeric IgA and is also expressed in most IgG-secreting cells. J chain-deficient mice have normal serum IgM and IgG levels but markedly elevated serum IgA. Although polymeric IgA was present in the mutant mice, a larger proportion of their serum IgA was monomeric than was found in wild-type mouse serum. Bile and fecal IgA levels were decreased in J chain-deficient mice compared with wild-type mice, suggesting inefficient transport of J chain-deficient IgA by hepatic polymeric immunoglobulin receptors (pIgR). The pIgR-mediated transport of serum-derived IgA from wild-type and mutant mice was assessed in Madin-Darby canine kidney (MDCK) cells transfected with the pIgR. These studies revealed selective transport by pIgR-expressing MDCK cells of wild-type IgA but not J chain-deficient IgA. We conclude that although the J chain is not required for IgA dimerization, it does affect the efficiency of polymerization or have a role in maintaining IgA dimer stability. Furthermore, the J chain is essential for efficient hepatic pIgR transport of IgA.

Published

1995

22. Characterization of soluble factors that induce the cytolytic activity and the expression of T cell growth factor receptors of a T cell hybrid.

Author

Erard, F, Corthesy, P, Smith, K A, Fiers, W, Conzelmann, A, and Nabholz, M

Abstract

A rat X mouse T cell hybrid (PC60) proliferates in the absence of T cell growth factor (TCGF) and its cytolytic activity can be induced by culture in mixed leukocyte culture supernatants or concanavalin A-activated rat spleen cell supernatant (CS) to lyse 51Cr-labeled tumor target cells. To characterize the factor(s) responsible for this reversible induction, serum-free CS was fractionated by reverse phase high performance liquid chromatography and by phenyl-Sepharose chromatography. A cytotoxicity-inducing activity (CIA) was separated from TCGF and macrophage-activating factor/interferon-gamma. CIA was found to be a macromolecule with an apparent molecular weight of 12,000-18,000 and a pI of 5.0 and 6.2. Its activity on PC60 cells depended on the addition of TCGF. Thus TCGF may have other effects on T cells than the induction of entry into cell cycle. The number of TCGF surface receptors on PC60 cells was measured using purified 3H-TCGF. TCGF receptors were undetectable on noninduced cells but appeared during induction. The expression of TCGF receptors was not induced either by TCGF or by CIA-containing supernatants or fractions alone, only by a combination of both. These results show that TCGF plays a role in the regulation of the expression of its own receptors.

Published

1984

23. Na(+)-K(+)-ATPase gene expression during in vitro development of rat fetal forebrain

Author

Corthesy-Theulaz, I., Merillat, A. M., Honegger, P., and Rossier, B. C.

Abstract

The existence of at least three isoforms of Na(+)-K(+)-ATPase in adult brain tissues [alpha 1, kidney type; alpha 2 [or alpha(+)]; alpha 3] suggests that these genes might be regulated in a cell-specific and time-dependent manner during development. We have studied this question in serum-free aggregating cell cultures of mechanically dissociated rat fetal telencephalon. At the protein level, the relative rate of synthesis of the pool of alpha 1-, alpha 2-, and alpha 3-subunits increased approximately twofold over 15 days of culture, leading to a marked increase in the immunochemical pool of alpha-subunits as measured by a panspecific polyclonal antibody. Concomitantly, Na(+)-K(+)-ATPase enzyme-specific activity increased three- (lower forebrain) to sixfold (upper forebrain). The transcripts of all three alpha-isoforms and beta-subunit were detected in vitro in similar proportion to the level observed in vivo. alpha 3-mRNA (3.7 kb) was more abundant than alpha 1 (3.7 kb) or alpha 2 (5.3 and 3.4 kb). Cytosine arabinoside (0.4 microM) and cholera toxin (0.1 microM) were used to selectively eliminate glial cells or neurons, respectively. It was found that alpha 2-mRNA is predominantly transcribed in glial cell cultures, whereas alpha 3- and beta 1-mRNA (2.7, 2.3, and 1.8 kb) are predominant in neuronal cultures.

Published

1990

24. Expression of epithelial Na channels in Xenopus oocytes.

Author

Palmer, L G, Corthesy-Theulaz, I, Gaeggeler, H P, Kraehenbuhl, J P, and Rossier, B

Abstract

Epithelial Na channel activity was expressed in oocytes from Xenopus laevis after injection of mRNA from A6 cells, derived from Xenopus kidney. Poly A(+) RNA was extracted from confluent cell monolayers grown on either plastic or permeable supports. 1-50 ng RNA was injected into stage 5-6 oocytes. Na channel activity was assayed as amiloride-sensitive current (INa) under voltage-clamp conditions 1-3 d after injection. INa was not detectable in noninjected or water-injected oocytes. This amiloride-sensitive pathway induced by the mRNA had a number of characteristics in common with that in epithelial cells, including (a) high selectivity for Na over K, (b) high sensitivity to amiloride with an apparent K1 of approximately 100 nM, (c) saturation with respect to external Na with an apparent Km of approximately 10 mM, and (d) a time-dependent activation of current with hyperpolarization of the oocyte membrane. Expression of channel activity was temperature dependent, being slow at 19 degrees C but much more rapid at 25 degrees C. Fractionation of mRNA on a sucrose density gradient revealed that the species of RNA inducing channel activity had a sedimentation coefficient of approximately 17 S. Treatment of filter-grown cells with 300 nM aldosterone for 24 h increased Na transport in the A6 cells by up to fivefold but did not increase the ability of mRNA isolated from those cells to induce channel activity in oocytes. The apparent abundance of mRNA coding for channel activity was 10-fold less in cells grown on plastic than in those grown on filters, but was increased two- to threefold by aldosterone.

Published

1990

25. Mouse interleukin-2 receptor alpha gene expression. Delimitation of cis-acting regulatory elements in transgenic mice and by mapping of DNase-I hypersensitive sites

Author

Soldaini, E., Pla, M., Beermann, F., Espel, E., Corthesy, P., Barange, S., Waanders, G. A., MacDonald, H. R., and Nabholz, M.

Abstract

The alpha chain of the interleukin-2 receptor (IL-2R alpha) is a key regulator of lymphocyte proliferation. To analyze the mechanisms controlling its expression in normal cells, we used the 5'-flanking region (base pairs -2539/+93) of the mouse gene to drive chloramphenicol acetyltransferase expression in four transgenic mouse lines. Constitutive transgene activity was restricted to lymphoid organs. In mature T lymphocytes, transgene and endogenous IL-2R alpha gene expression was stimulated by concanavalin A and up-regulated by IL-2 with very similar kinetics. In thymic T cell precursors, IL-1 and IL-2 cooperatively induced transgene and IL-2R alpha gene expression. These results show that regulation of the endogenous IL-2R alpha gene occurs mainly at the transcriptional level. They demonstrate that cis-acting elements in the 5'-flanking region present in the transgene confer correct tissue specificity and inducible expression in mature T cells and their precursors in response to antigen, IL-1, and IL-2. In a complementary approach, we screened the 5' end of the endogenous IL-2R alpha gene for DNase-I hypersensitive sites. We found three lymphocyte specific DNase-I hypersensitive sites. Two, at -0.05 and -5.3 kilobase pairs, are present in resting T cells. A third site appears at -1.35 kilobase pairs in activated T cells. It co-localizes with IL-2-responsive elements identified by transient transfection experiments.

26. Mouse interleukin-2 receptor alpha gene expression. Interleukin-1 and interleukin-2 control transcription via distinct cis-acting elements

Author

Sperisen, P., Wang, S. M., Soldaini, E., Pla, M., Rusterholz, C., Bucher, P., Corthesy, P., Reichenbach, P., and Nabholz, M.

Abstract

We have shown that interleukin-1 (IL-1) and IL-2 control IL-2 receptor alpha (IL-2R alpha) gene transcription in CD4-CD8- murine T lymphocyte precursors. Here we map the cis-acting elements that mediate interleukin responsiveness of the mouse IL-2R alpha gene using a thymic lymphoma-derived hybridoma (PC60). The transcriptional response of the IL-2R alpha gene to stimulation by IL-1 + IL-2 is biphasic. IL-1 induces a rapid, protein synthesis-independent appearance of IL-2R alpha mRNA that is blocked by inhibitors of NF-kappa B activation. It also primes cells to become IL-2 responsive and thereby prepares the second phase, in which IL-2 induces a 100-fold further increase in IL-2R alpha transcripts. Transient transfection experiments show that several elements in the promoter-proximal region of the IL-2R alpha gene contribute to IL-1 responsiveness, most importantly an NF-kappa B site conserved in the human and mouse gene. IL-2 responsiveness, on the other hand, depends on a 78-nucleotide segment 1.3 kilobases upstream of the major transcription start site. This segment functions as an IL-2-inducible enhancer and lies within a region that becomes DNase I hypersensitive in normal T cells in which IL-2R alpha expression has been induced. IL-2 responsiveness requires three distinct elements within the enhancer. Two of these are potential binding sites for STAT proteins.

27. Antigens of activated rat T lymphocytes including a molecule of 50,000 Mr detected only on CD4 positive T blasts

Author

PATERSON, D, primary, JEFFERIES, W, additional, GREEN, J, additional, BRANDON, M, additional, CORTHESY, P, additional, PUKLAVEC, M, additional, and WILLIAMS, A, additional

Published

1987

28. Interleukin 2 is both necessary and sufficient for the growth and differentiation of lectin-stimulated cytolytic T lymphocyte precursors.

Author

Erard, F, primary, Corthesy, P, additional, Nabholz, M, additional, Lowenthal, J W, additional, Zaech, P, additional, Plaetinck, G, additional, and MacDonald, H R, additional

Published

1985

29. Molecular study of H. pylori-epithelial cell interaction: A novel in vitrosystem basedon differential culture conditions and cell polarity

Author

Cottet, Sandra, Corthesy-Theulaz, Irene E., Kraehenbuhl, Jean-Pierre, and Corthesy, Blaise E.

Published

2000

30. Chronic Gastrointestinal Inflammation Induces Anxiety-Like Behavior and Alters Central Nervous System Biochemistry in Mice.

Author

Bercik, Premysl, Verdu, Elena F., Foster, Jane A., Macri, Joseph, Potter, Murray, Huang, Xiaxing, Malinowski, Paul, Jackson, Wendy, Blennerhassett, Patricia, Neufeld, Karen A., Lu, Jun, Khan, Waliul I., Corthesy–Theulaz, Irene, Cherbut, Christine, Bergonzelli, Gabriela E., and Collins, Stephen M.

Subjects

GASTROENTERITIS, ANXIETY, CENTRAL nervous system, BIOCHEMISTRY, LABORATORY mice, TUMOR necrosis factors, MESSENGER RNA

Abstract

Background & Aims: Clinical and preclinical studies have associated gastrointestinal inflammation and infection with altered behavior. We investigated whether chronic gut inflammation alters behavior and brain biochemistry and examined underlying mechanisms. Methods: AKR mice were infected with the noninvasive parasite Trichuris muris and given etanercept, budesonide, or specific probiotics. Subdiaphragmatic vagotomy was performed in a subgroup of mice before infection. Gastrointestinal inflammation was assessed by histology and quantification of myeloperoxidase activity. Serum proteins were measured by proteomic analysis, circulating cytokines were measured by fluorescence activated cell sorting array, and serum tryptophan and kynurenine were measured by liquid chromatography. Behavior was assessed using light/dark preference and step-down tests. In situ hybridization was used to assess brain-derived neurotrophic factor (BDNF) expression in the brain. Results: T muris caused mild to moderate colonic inflammation and anxiety-like behavior that was associated with decreased hippocampal BDNF messenger RNA (mRNA). Circulating tumor necrosis factor-α and interferon-γ, as well as the kynurenine and kynurenine/tryptophan ratio, were increased. Proteomic analysis showed altered levels of several proteins related to inflammation and neural function. Administration of etanercept, and to a lesser degree of budesonide, normalized behavior, reduced cytokine and kynurenine levels, but did not influence BDNF expression. The probiotic Bifidobacterium longum normalized behavior and BDNF mRNA but did not affect cytokine or kynurenine levels. Anxiety-like behavior was present in infected mice after vagotomy. Conclusions: Chronic gastrointestinal inflammation induces anxiety-like behavior and alters central nervous system biochemistry, which can be normalized by inflammation-dependent and -independent mechanisms, neither of which requires the integrity of the vagus nerve. [Copyright &y& Elsevier]

Published

2010

31. Strain-dependent effects of probiotics on intestinal muscle dysfunction in an animal model of post-infective irritable bowel syndrome

Author

Verdu, Elena F., Bercik, Premysl, Blennerhassett, Patricia, Huang, Xian Xi, Bergonzelli, Gabriela, Corthesy-Theulaz, Irene, and Collins, Stephen M.

Published

2003

32. Molecular definition of the role of secretory component in secretory IgA-mediated protection at mucosal surfaces

Author

Corthesy, Blaise and Phalipon, Armelle

Published

2002

33. BALB/c mice immunized with UreB and CT require the presence of neutrophils during the second week post-infection to be protected against Helicobacter

Author

Isler, P., Tachinni-Cottier, F., Bachmann, D., and Corthesy-Theulaz, I.

Published

2001

34. Evidence for high Helicobacter pylori mucosal specific IgG secretion in autoimmune gastritis

Author

Dorta, G.O., Antos, D., Radke, J., Miehlke, S., Martinek, J., Corthesy-Theulaz, I., Blum, A., Michetti, P., Isler, P., Stolte, M., Claeys, D., and Bayerdoerffer, E.

Published

2001

35. Evidence for high Helicobacter pylorimucosal specific IgG secretion in autoimmune gastritis

Author

Dorta, Gian Oh, Antos, David, Radke, Joergen, Miehlke, Stefan, Martinek, Jan, Corthesy-Theulaz, Irene, Blum, Andre, Michetti, Pierre, Isler, Patrick, Stolte, Manfred, Claeys, Dirk, and Bayerdoerffer, Ekkehard

Published

2001

36. Live vaccination with Salmonella typhimuriumexpressing H. pyloriurease: A delicate balance between protection and safety

Author

Isler, Patrick, Bachmann, Daniel, Blum, Andre L., and Corthesy-Theulaz, Irene E.

Published

2000

37. A thiolase inhibitory peptide enters h. pylori cells and induces death: A new peptide-based therapeutical approach?

Author

Marin-Kuan, Maricel, Bergonzelli, Gabriela E., Houimel, Mehdi, Mach, Jean-Pierre, Blum, Andre L., and Corthesy, Irene E.

Published

2000

38. Mouse IL-2Rα gene regulation by IL-1 and IL-2

Author

Soldaini, E., Sperisen, P., Pla, M., Wang, S.-M., Rusterholz, C., Reichenbach, P., Corthesy, P., Wilson, A., Beermann, F., and Nabholz, M.

Published

1994

39. Fine structural variations of alphabetaTCRs selected by vaccination with natural versus altered self-antigen in melanoma patients.

Author

Wieckowski S, Baumgaertner P, Corthesy P, Voelter V, Romero P, Speiser DE, and Rufer N

Subjects

Amino Acid Sequence, Antigens, Neoplasm therapeutic use, Autoantigens therapeutic use, Base Sequence, Cancer Vaccines therapeutic use, HLA-A Antigens immunology, HLA-A2 Antigen immunology, Humans, Immunotherapy, MART-1 Antigen, Melanoma immunology, Molecular Sequence Data, Neoplasm Proteins therapeutic use, Prospective Studies, Protein Conformation, Receptors, Antigen, T-Cell, alpha-beta immunology, Sequence Alignment, Skin Neoplasms immunology, Antigens, Neoplasm immunology, Autoantigens immunology, CD8-Positive T-Lymphocytes immunology, Cancer Vaccines immunology, Melanoma therapy, Neoplasm Proteins immunology, Receptors, Antigen, T-Cell, alpha-beta chemistry, Skin Neoplasms therapy

Abstract

Immunotherapy of cancer is often performed with altered "analog" peptide Ags optimized for HLA class I binding, resulting in enhanced immunogenicity, but the induced T cell responses require further evaluation. Recently, we demonstrated fine specificity differences and enhanced recognition of naturally presented Ag by T cells after vaccination with natural Melan-A/MART-1 peptide, as compared with analog peptide. In this study, we compared the TCR primary structures of 1489 HLA-A*0201/Melan-A(26-35)-specific CD8 T cells derived from both cohorts of patients. Although a strong preference for TRAV12-2 segment usage was present in nearly all patients, usage of particular TRAJ gene segments and CDR3alpha composition differed slightly after vaccination with natural vs analog peptide. Moreover, TCR beta-chain repertoires were broader after natural than analog peptide vaccination. In all patients, we observed a marked conservation of the CDR3beta amino acid composition with recurrent sequences centered on a glycyl-leucyl/valyl/alanyl-glycyl motif. In contrast to viral-specific TCR repertoires, such "public" motifs were primarily expressed by nondominant T cell clonotypes, which contrasted with "private" CDR3beta signatures frequently found in T cell clonotypes that dominated repertoires of individual patients. Interestingly, no differences in functional avidity were observed between public and private T cell clonotypes. Collectively, our data indicate that T cell repertoires generated against natural or analog Melan-A peptide exhibited slightly distinct but otherwise overlapping and structurally conserved TCR features, suggesting that the differences in binding affinity/avidity of TCRs toward pMHC observed in the two cohorts of patients are caused by subtle structural TCR variations.

Published

2009

40. Clonotype selection and composition of human CD8 T cells specific for persistent herpes viruses varies with differentiation but is stable over time.

Author

Iancu EM, Corthesy P, Baumgaertner P, Devevre E, Voelter V, Romero P, Speiser DE, and Rufer N

Subjects

Adult, CD8-Positive T-Lymphocytes classification, Cancer Vaccines chemical synthesis, Cancer Vaccines genetics, Cancer Vaccines immunology, Cell Differentiation genetics, Cells, Cultured, Cellular Senescence genetics, Clone Cells, Cytomegalovirus pathogenicity, Cytomegalovirus Infections immunology, Cytomegalovirus Infections prevention & control, Cytomegalovirus Infections virology, Epitopes, T-Lymphocyte chemistry, Epitopes, T-Lymphocyte genetics, Epstein-Barr Virus Infections immunology, Epstein-Barr Virus Infections prevention & control, Epstein-Barr Virus Infections virology, Gene Expression Regulation, Viral immunology, Herpesvirus 4, Human pathogenicity, Herpesvirus Vaccines chemical synthesis, Herpesvirus Vaccines genetics, Herpesvirus Vaccines immunology, Humans, Middle Aged, Phosphoproteins chemistry, Phosphoproteins genetics, Phosphoproteins immunology, Receptors, Antigen, T-Cell chemistry, Receptors, Antigen, T-Cell genetics, Receptors, Antigen, T-Cell metabolism, Receptors, Antigen, T-Cell, alpha-beta chemistry, Receptors, Antigen, T-Cell, alpha-beta genetics, Receptors, Antigen, T-Cell, alpha-beta immunology, Time Factors, Trans-Activators chemistry, Trans-Activators genetics, Trans-Activators immunology, Viral Matrix Proteins chemistry, Viral Matrix Proteins genetics, Viral Matrix Proteins immunology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes virology, Cell Differentiation immunology, Cellular Senescence immunology, Cytomegalovirus immunology, Epitopes, T-Lymphocyte immunology, Herpesvirus 4, Human immunology

Abstract

Protection from reactivation of persistent herpes virus infection is mediated by Ag-specific CD8 T cell responses, which are highly regulated by still poorly understood mechanisms. In this study, we analyzed differentiation and clonotypic dynamics of EBV- and CMV-specific T cells from healthy adults. Although these T lymphocytes included all subsets, from early-differentiated (EM/CD28(pos)) to late-differentiated (EMRA/CD28(neg)) stages, they varied in the sizes/proportions of these subsets. In-depth clonal composition analyses revealed TCR repertoires, which were highly restricted for CMV- and relatively diverse for EBV-specific cells. Virtually all virus-specific clonotypes identified in the EMRA/CD28(neg) subset were also found within the pool of less differentiated "memory" cells. However, striking differences in the patterns of dominance were observed among these subsets, because some clonotypes were selected with differentiation while others were not. Late-differentiated CMV-specific clonotypes were mostly characterized by TCR with lower dependency on CD8 coreceptor interaction. Yet all clonotypes displayed similar functional avidities, suggesting a compensatory role of CD8 in the clonotypes of lower TCR avidity. Importantly, clonotype selection and composition of each virus-specific subset upon differentiation was highly preserved over time, with the presence of the same dominant clonotypes at specific differentiation stages within a period of 4 years. Remarkably, clonotypic distribution was stable not only in late-differentiated but also in less-differentiated T cell subsets. Thus, T cell clonotypes segregate with differentiation, but the clonal composition once established is kept constant for at least several years. These findings reveal novel features of the highly sophisticated control of steady state protective T cell activity in healthy adults.

Published

2009

41. Dominant human CD8 T cell clonotypes persist simultaneously as memory and effector cells in memory phase.

Author

Touvrey C, Derré L, Devevre E, Corthesy P, Romero P, Rufer N, and Speiser DE

Subjects

CD28 Antigens analysis, Cell Differentiation, Clone Cells immunology, Granzymes analysis, Humans, Immunophenotyping, Interleukin-7 Receptor alpha Subunit analysis, Perforin analysis, CD8-Positive T-Lymphocytes immunology, Cytotoxicity, Immunologic, Immunologic Memory

Abstract

The adaptive immune system plays a critical role in protection at the time of secondary infection. It does so through the rapid and robust reactivation of memory T cells which are maintained long-term, in a phenotypically heterogeneous state, following their primary encounter with Ag. Although most HLA-A*0201/influenza matrix protein(58-66)-specific CD8 T cells from healthy donors display characteristics typical of memory T cells, through our extensive phenotypic analysis we have further shown that up to 20% of these cells express neither the IL-7 receptor CD127 nor the costimulatory molecule CD28. In contrast to the majority of CD28(pos) cells, granzyme B and perforin were frequently expressed by the CD28(neg) cells, suggesting that they are effector cells. Indeed, these cells were able to kill target cells, in an Ag-specific manner, directly ex vivo. Thus, our findings demonstrate the remarkable long-term persistence in healthy humans of not only influenza-specific memory cells, but also of effector T cells. We further observed that granzyme B expression in influenza-specific CD8 T cells paralleled levels in the total CD8 T cell population, suggestive of Ag-nonspecific bystander activation. Sequencing of TCR alpha- and beta-chains showed that the TCR repertoire specific for this epitope was dominated by one, or a few, T cell clonotype per healthy donor. Moreover, our sequencing analysis revealed, for the first time in humans, that identical clonotypes can coexist as both memory and effector T cells, thereby supporting the principle of multipotent clonotypic differentiation.

Published

2009

42. In Vivo Persistence of Codominant Human CD8+ T Cell Clonotypes Is Not Limited by Replicative Senescence or Functional Alteration.

Author

Derré L, Bruyninx M, Baumgaertner P, Devevre E, Corthesy P, Touvrey C, Mahnke YD, Pircher H, Voelter V, Romero P, Speiser DE, and Rufer N

Subjects

CD8-Positive T-Lymphocytes pathology, Cell Proliferation, Epitopes, T-Lymphocyte immunology, Follow-Up Studies, HLA-A2 Antigen immunology, Humans, Lymph Nodes immunology, Lymph Nodes pathology, Lymphatic Metastasis, Melanoma pathology, Melanoma therapy, Middle Aged, Neoplasm Proteins immunology, Receptors, Antigen, T-Cell immunology, Skin Neoplasms pathology, Skin Neoplasms therapy, Telomere immunology, Time Factors, Viruses immunology, Acetyltransferases immunology, Antigens, Neoplasm immunology, CD8-Positive T-Lymphocytes immunology, Cell Differentiation immunology, Cellular Senescence immunology, Immunologic Memory, Melanoma immunology, Peptides immunology, Skin Neoplasms immunology

Abstract

T cell responses to viral epitopes are often composed of a small number of codominant clonotypes. In this study, we show that tumor Ag-specific T cells can behave similarly. In a melanoma patient with a long lasting HLA-A2/NY-ESO-1-specific T cell response, reaching 10% of circulating CD8 T cells, we identified nine codominant clonotypes characterized by individual TCRs. These clonotypes made up almost the entire pool of highly differentiated effector cells, but only a fraction of the small pool of less differentiated "memory" cells, suggesting that the latter serve to maintain effector cells. The different clonotypes displayed full effector function and expressed TCRs with similar functional avidity. Nevertheless, some clonotypes increased, whereas others declined in numbers over the observation period of 6 years. One clonotype disappeared from circulating blood, but without preceding critical telomere shortening. In turn, clonotypes with increasing frequency had accelerated telomere shortening, correlating with strong in vivo proliferation. Interestingly, the final prevalence of the different T cell clonotypes in circulation was anticipated in a metastatic lymph node withdrawn 2 years earlier, suggesting in vivo clonotype selection driven by metastases. Together, these data provide novel insight in long term in vivo persistence of T cell clonotypes associated with continued cell turnover but not replicative senescence or functional alteration.

Published

2007

43. Four functionally distinct populations of human effector-memory CD8+ T lymphocytes.

Author

Romero P, Zippelius A, Kurth I, Pittet MJ, Touvrey C, Iancu EM, Corthesy P, Devevre E, Speiser DE, and Rufer N

Subjects

Adult, Aged, CD28 Antigens genetics, Cell Differentiation, Female, Flow Cytometry, Gene Expression Profiling, Granzymes genetics, Humans, Interleukin-7 Receptor alpha Subunit analysis, Male, Membrane Glycoproteins genetics, Middle Aged, Perforin, Pore Forming Cytotoxic Proteins genetics, RNA, Messenger analysis, Receptors, Antigen, T-Cell genetics, Receptors, CCR6, Receptors, Chemokine analysis, Receptors, Chemokine genetics, Receptors, Interleukin-7 analysis, Telomere metabolism, Tumor Necrosis Factor Receptor Superfamily, Member 7 genetics, CD8-Positive T-Lymphocytes classification, CD8-Positive T-Lymphocytes immunology, Immunologic Memory, T-Lymphocyte Subsets classification, T-Lymphocyte Subsets immunology

Abstract

In humans, the pathways of memory and effector T cell differentiation remain poorly defined. We have dissected the functional properties of ex vivo effector-memory (EM) CD45RA-CCR7- T lymphocytes present within the circulating CD8+ T cell pool of healthy individuals. Our studies show that EM T cells are heterogeneous and are subdivided based on differential CD27 and CD28 expression into four subsets. EM(1) (CD27+CD28+) and EM(4) (CD27-CD28+) T cells express low levels of effector mediators such as granzyme B and perforin and high levels of CD127/IL-7Ralpha. EM(1) cells also have a relatively short replicative history and display strong ex vivo telomerase activity. Therefore, these cells are closely related to central-memory (CD45RA-CCR7+) cells. In contrast, EM(2) (CD27+CD28-) and EM(3) (CD27-CD28-) cells express mediators characteristic of effector cells, whereby EM(3) cells display stronger ex vivo cytolytic activity and have experienced larger numbers of cell divisions, thus resembling differentiated effector (CD45RA+CCR7-) cells. These data indicate that progressive up-regulation of cytolytic activity and stepwise loss of CCR7, CD28, and CD27 both characterize CD8+ T cell differentiation. Finally, memory CD8+ T cells not only include central-memory cells but also EM(1) cells, which differ in CCR7 expression and may therefore confer memory functions in lymphoid and peripheral tissues, respectively.

Published

2007

44. A novel approach to characterize clonality and differentiation of human melanoma-specific T cell responses: spontaneous priming and efficient boosting by vaccination.

Author

Speiser DE, Baumgaertner P, Barbey C, Rubio-Godoy V, Moulin A, Corthesy P, Devevre E, Dietrich PY, Rimoldi D, Liénard D, Cerottini JC, Romero P, and Rufer N

Subjects

Antigen Presentation immunology, Antigens, Neoplasm, CD8-Positive T-Lymphocytes metabolism, CD8-Positive T-Lymphocytes pathology, Cancer Vaccines administration & dosage, Clone Cells, Cytotoxicity Tests, Immunologic, Disease Progression, Epitopes, T-Lymphocyte blood, Humans, Immunodominant Epitopes administration & dosage, Immunodominant Epitopes immunology, Lymphatic Metastasis immunology, Lymphatic Metastasis pathology, Lymphocyte Count, MART-1 Antigen, Melanoma pathology, Melanoma secondary, Neoplasm Proteins blood, Receptors, Antigen, T-Cell analysis, Receptors, Antigen, T-Cell blood, Receptors, Antigen, T-Cell metabolism, Time Factors, Vaccines, Subunit administration & dosage, Vaccines, Subunit immunology, CD8-Positive T-Lymphocytes immunology, Cancer Vaccines immunology, Cell Differentiation immunology, Epitopes, T-Lymphocyte immunology, Immunization, Secondary, Melanoma immunology, Melanoma therapy, Neoplasm Proteins immunology

Abstract

Despite major progress in T lymphocyte analysis in melanoma patients, TCR repertoire selection and kinetics in response to tumor Ags remain largely unexplored. In this study, using a novel ex vivo molecular-based approach at the single-cell level, we identified a single, naturally primed T cell clone that dominated the human CD8(+) T cell response to the Melan-A/MART-1 Ag. The dominant clone expressed a high-avidity TCR to cognate tumor Ag, efficiently killed tumor cells, and prevailed in the differentiated effector-memory T lymphocyte compartment. TCR sequencing also revealed that this particular clone arose at least 1 year before vaccination, displayed long-term persistence, and efficient homing to metastases. Remarkably, during concomitant vaccination over 3.5 years, the frequency of the pre-existing clone progressively increased, reaching up to 2.5% of the circulating CD8 pool while its effector functions were enhanced. In parallel, the disease stabilized, but subsequently progressed with loss of Melan-A expression by melanoma cells. Collectively, combined ex vivo analysis of T cell differentiation and clonality revealed for the first time a strong expansion of a tumor Ag-specific human T cell clone, comparable to protective virus-specific T cells. The observed successful boosting by peptide vaccination support further development of immunotherapy by including strategies to overcome immune escape.

Published

2006