Your search keyword '"Lantz, Olivier"' showing total 23 results

1. Protective effect of TCR-mediated MAIT cell activation during experimental autoimmune encephalomyelitis.

Author

Walkenhorst, Mark, Sonner, Jana K., Meurs, Nina, Engler, Jan Broder, Bauer, Simone, Winschel, Ingo, Woo, Marcel S., Raich, Lukas, Winkler, Iris, Vieira, Vanessa, Unger, Lisa, Salinas, Gabriela, Lantz, Olivier, Friese, Manuel A., and Willing, Anne

Abstract

Mucosal-associated invariant T (MAIT) cells express semi-invariant T cell receptors (TCR) for recognizing bacterial and yeast antigens derived from riboflavin metabolites presented on the non-polymorphic MHC class I-related protein 1 (MR1). Neuroinflammation in multiple sclerosis (MS) is likely initiated by autoreactive T cells and perpetuated by infiltration of additional immune cells, but the precise role of MAIT cells in MS pathogenesis remains unknown. Here, we use experimental autoimmune encephalomyelitis (EAE), a mouse model of MS, and find an accumulation of MAIT cells in the inflamed central nervous system (CNS) enriched for MAIT17 (RORγt+) and MAIT1/17 (T-bet+RORγt+) subsets with inflammatory and protective features. Results from transcriptome profiling and Nur77GFP reporter mice show that these CNS MAIT cells are activated via cytokines and TCR. Blocking TCR activation with an anti-MR1 antibody exacerbates EAE, whereas enhancing TCR activation with the cognate antigen, 5-(2-oxopropylideneamino)−6-D-ribitylaminouracil, ameliorates EAE severity, potentially via the induction of amphiregulin (AREG). In summary, our findings suggest that TCR-mediated MAIT cell activation is protective in CNS inflammation, likely involving an induction of AREG. Mucosal-associated invariant T (MAIT) cells mediate protection from pathogens, but their role in autoimmunity is unclear. Here the authors show that, in a mouse experimental autoimmune encephalomyelitis model, MAIT cells accumulate in the inflamed central nervous system and serve protective functions when activated via their T cell receptor. [ABSTRACT FROM AUTHOR]

Published

2024

2. Mucosal-associated invariant T cells contribute to suppression of inflammatory myeloid cells in immune-mediated kidney disease.

Author

Gnirck, Ann-Christin, Philipp, Marie-Sophie, Waterhölter, Alex, Wunderlich, Malte, Shaikh, Nikhat, Adamiak, Virginia, Henneken, Lena, Kautz, Tobias, Xiong, Tingting, Klaus, Daniela, Tomczyk, Pascal, Al-Bahra, Mohamad M., Menche, Dirk, Walkenhorst, Mark, Lantz, Olivier, Willing, Anne, Friese, Manuel A., Huber, Tobias B., Krebs, Christian F., and Panzer, Ulf

Subjects

MYELOID cells, KIDNEY diseases, T cells, VITAMIN B2, MACROPHAGES, DNA fingerprinting

Abstract

Mucosal-associated invariant T (MAIT) cells have been implicated in various inflammatory diseases of barrier organs, but so far, their role in kidney disease is unclear. Here we report that MAIT cells that recognize their prototypical ligand, the vitamin B2 intermediate 5-OP-RU presented by MR1, reside in human and mouse kidneys. Single cell RNAseq analysis reveals several intrarenal MAIT subsets, and one, carrying the genetic fingerprint of tissue-resident MAIT17 cells, is activated and expanded in a murine model of crescentic glomerulonephritis (cGN). An equivalent subset is also present in kidney biopsies of patients with anti-neutrophil cytoplasmatic antibody (ANCA)-associated cGN. MAIT cell-deficient MR1 mice show aggravated disease, whereas B6-MAITCAST mice, harboring higher MAIT cell numbers, are protected from cGN. The expanded MAIT17 cells express anti-inflammatory mediators known to suppress cGN, such as CTLA-4, PD-1, and TGF-β. Interactome analysis predicts CXCR6 – CXCL16-mediated cross-talk with renal mononuclear phagocytes, known to drive cGN progression. In line, we find that cGN is aggravated upon CXCL16 blockade. Finally, we present an optimized 5-OP-RU synthesis method which we apply to attenuating cGN in mice. In summary, we propose that CXCR6+ MAIT cells might play a protective role in cGN, implicating them as a potential target for anti-inflammatory therapies. Mucosal associated invariant T (MAIT) cells reside in barrier organs, but their contribution to inflammatory processes in the kidneys is not fully known. Here authors find by single cell RNA sequencing that among the different MAIT cell subtypes found at steady state, a population with MAIT17 signature is expanded in both human crescentic glomerulonephritis and its mouse model, and these cells may play protective role in the disease. [ABSTRACT FROM AUTHOR]

Published

2023

3. Immunohistochemical characterisation of the immune landscape in primary uveal melanoma and liver metastases.

Author

Mariani, Pascale, Torossian, Nouritza, van Laere, Steven, Vermeulen, Peter, de Koning, Leanne, Roman-Roman, Sergio, Lantz, Olivier, Rodrigues, Manuel, Stern, Marc-Henri, Gardrat, Sophie, Lesage, Laetitia, Champenois, Gabriel, Nicolas, André, Matet, Alexandre, Cassoux, Nathalie, Servois, Vincent, Romano, Emanuela, Piperno-Neumann, Sophie, Lugassy, Claire, and Barnhill, Raymond

Abstract

Background: The immune landscape of uveal melanoma liver metastases (UMLM) has not been sufficiently studied. Methods: Immune cell infiltrates (ICIs), PD-1 and PD-L1 were characterised in 62 UMLM and 28 primary uveal melanomas (PUM). ICI, PD-1 and PD-L1 were scored as: (1) % tumoral area occupied by tumour-infiltrating lymphocytes or macrophages (TILs, TIMs) and (2) % perTumoral (perT) area. ICIs and other variables including histopathologic growth patterns (HGPs), replacement and desmoplastic, of UMLM were analysed for their prognostic value. Results: ICIs recognised by haematoxylin-eosin-saffron (HES) and IHC (e.g., T cells (CD3), B cells (CD20). Macrophages (CD68), (CD163), were primarily localised to the perT region in PUM and UMLM and were more conspicuous in UMLM. HES, CD3, CD4, FoxP3, CD8, CD20, PD-1 TILs were scant (<5%). TIMs were more frequent, particularly in UMLM than in PUM. Both CD68+ TIMs and HGPs remained significant on multivariate analysis, influencing overall (OS) and metastasis-specific overall survival (MSOS). CD68 + , CD163+ and CD20+ perT infiltrates in UMLM predicted increased OS and MSOS on univariate analysis. Conclusions: TILs and PD-L1 have no predictive value in PUM or UMLM. CD68+ and CD163+TIMs, CD20+ perT lymphocytes, and HGPs are important prognostic factors in UMLMs. [ABSTRACT FROM AUTHOR]

Published

2023

4. MAIT cell inhibition promotes liver fibrosis regression via macrophage phenotype reprogramming.

Author

Mabire, Morgane, Hegde, Pushpa, Hammoutene, Adel, Wan, Jinghong, Caër, Charles, Sayegh, Rola Al, Cadoux, Mathilde, Allaire, Manon, Weiss, Emmanuel, Thibault-Sogorb, Tristan, Lantz, Olivier, Goodhardt, Michèle, Paradis, Valérie, de la Grange, Pierre, Gilgenkrantz, Hélène, and Lotersztajn, Sophie

Subjects

HEPATIC fibrosis, NON-alcoholic fatty liver disease, MACROPHAGES, PHENOTYPES, MACROPHAGE activation, IMMUNOGLOBULINS

Abstract

Recent data have shown that liver fibrosis can regress even at later stages of cirrhosis and shifting the immune response from pro-inflammatory towards a resolutive profile is considered as a promising option. The immune regulatory networks that govern the shift of the inflammatory phenotype and thus potential reversal of liver fibrosis are lesser known. Here we show that in precision-cut human liver slices obtained from patients with end-stage fibrosis and in mouse models, inhibiting Mucosal-Associated Invariant T (MAIT) cells using pharmacological or antibody-driven approaches, limits fibrosis progression and even regresses fibrosis, following chronic toxic- or non-alcoholic steatohepatitis (NASH)-induced liver injury. Mechanistic studies, combining RNA sequencing, in vivo functional studies (performed in male mice) and co-culture experiments indicate that disruption of the MAIT cell-monocyte/macrophage interaction results in resolution of fibrosis both by increasing the frequency of restorative Ly6Clo at the expenses of pro-fibrogenic Ly6Chi monocyte-derived macrophages and promoting an autophagic phenotype in both subsets. Thus, our data show that MAIT cell activation and the consequential phenotype shift of liver macrophages are important pathogenic features of liver fibrosis and could be targeted by anti-fibrogenic therapy. Liver cirrhosis is characterised by extensive fibrosis of the liver, and understanding the underpinning immunological processes is important in designing intervention. Here authors show that Mucosal-Associated Invariant T cells are instrumental to controlling the balance between profibrogenic and restorative macrophages and inhibiting their activation might reverse liver fibrosis. [ABSTRACT FROM AUTHOR]

Published

2023

5. PD-L1 and ICOSL discriminate human Secretory and Helper dendritic cells in cancer, allergy and autoimmunity.

Author

Hoffmann, Caroline, Noel, Floriane, Grandclaudon, Maximilien, Massenet-Regad, Lucile, Michea, Paula, Sirven, Philemon, Faucheux, Lilith, Surun, Aurore, Lantz, Olivier, Bohec, Mylene, Ye, Jian, Guo, Weihua, Rochefort, Juliette, Klijanienko, Jerzy, Baulande, Sylvain, Lecerf, Charlotte, Kamal, Maud, Le Tourneau, Christophe, Guillot-Delost, Maude, and Soumelis, Vassili

Subjects

T cells, CANCER cells, DENDRITIC cells, PROGRAMMED death-ligand 1, AUTOIMMUNITY, SQUAMOUS cell carcinoma

Abstract

Dendritic cells (DC) are traditionally classified according to their ontogeny and their ability to induce T cell response to antigens, however, the phenotypic and functional state of these cells in cancer does not necessarily align to the conventional categories. Here we show, by using 16 different stimuli in vitro that activated DCs in human blood are phenotypically and functionally dichotomous, and pure cultures of type 2 conventional dendritic cells acquire these states (termed Secretory and Helper) upon appropriate stimuli. PD-L1highICOSLlow Secretory DCs produce large amounts of inflammatory cytokines and chemokines but induce very low levels of T helper (Th) cytokines following co-culturing with T cells. Conversely, PD-L1lowICOSLhigh Helper DCs produce low levels of secreted factors but induce high levels and a broad range of Th cytokines. Secretory DCs bear a single-cell transcriptomic signature indicative of mature migratory LAMP3+ DCs associated with cancer and inflammation. Secretory DCs are linked to good prognosis in head and neck squamous cell carcinoma, and to response to checkpoint blockade in Melanoma. Hence, the functional dichotomy of DCs we describe has both fundamental and translational implications in inflammation and immunotherapy. Phenotypic and functional states of dendritic cells critically influence the outcome of cancer and inflammation. Authors here show by single cell transcriptomics and in vitro validation assays that dichotomous PD-L1 and ICOSL expression assign dendritic cells to secretory and helper functions, with respective predominance of inflammatory cytokine expression or T helper cytokine induction. [ABSTRACT FROM AUTHOR]

Published

2022

6. A DNA methylation-based liquid biopsy for triple-negative breast cancer.

Author

Cristall, Katrina, Bidard, Francois-Clement, Pierga, Jean-Yves, Rauh, Michael J., Popova, Tatiana, Sebbag, Clara, Lantz, Olivier, Stern, Marc-Henri, and Mueller, Christopher R.

Subjects

TRIPLE-negative breast cancer, DNA methylation, DNA sequencing, BLOOD testing, BIOMARKERS, HEMATOPOIESIS

Abstract

Here, we present a next-generation sequencing (NGS) methylation-based blood test called methylation DETEction of Circulating Tumour DNA (mDETECT) designed for the optimal detection and monitoring of metastatic triple-negative breast cancer (TNBC). Based on a highly multiplexed targeted sequencing approach, this assay incorporates features that offer superior performance and included 53 amplicons from 47 regions. Analysis of a previously characterised cohort of women with metastatic TNBC with limited quantities of plasma (<2 ml) produced an AUC of 0.92 for detection of a tumour with a sensitivity of 76% for a specificity of 100%. mDETECTTNBC was quantitative and showed superior performance to an NGS TP53 mutation-based test carried out on the same patients and to the conventional CA15-3 biomarker. mDETECT also functioned well in serum samples from metastatic TNBC patients where it produced an AUC of 0.97 for detection of a tumour with a sensitivity of 93% for a specificity of 100%. An assay for BRCA1 promoter methylation was also incorporated into the mDETECT assay and functioned well but its clinical significance is currently unclear. Clonal Hematopoiesis of Indeterminate Potential was investigated as a source of background in control subjects but was not seen to be significant, though a link to adiposity may be relevant. The mDETECTTNBC assay is a liquid biopsy able to quantitatively detect all TNBC cancers and has the potential to improve the management of patients with this disease. [ABSTRACT FROM AUTHOR]

Published

2021

7. Mucosal-associated invariant T cells promote inflammation and intestinal dysbiosis leading to metabolic dysfunction during obesity.

Author

Toubal, Amine, Kiaf, Badr, Beaudoin, Lucie, Cagninacci, Lucie, Rhimi, Moez, Fruchet, Blandine, da Silva, Jennifer, Corbett, Alexandra J., Simoni, Yannick, Lantz, Olivier, Rossjohn, Jamie, McCluskey, James, Lesnik, Philippe, Maguin, Emmanuelle, and Lehuen, Agnès

Subjects

T cells, ADIPOSE tissue physiology, T cell receptors, OBESITY, METABOLIC disorders, ADIPOSE tissues

Abstract

Obesity is associated with low-grade chronic inflammation promoting insulin-resistance and diabetes. Gut microbiota dysbiosis is a consequence as well as a driver of obesity and diabetes. Mucosal-associated invariant T cells (MAIT) are innate-like T cells expressing a semi-invariant T cell receptor restricted to the non-classical MHC class I molecule MR1 presenting bacterial ligands. Here we show that during obesity MAIT cells promote inflammation in both adipose tissue and ileum, leading to insulin resistance and impaired glucose and lipid metabolism. MAIT cells act in adipose tissue by inducing M1 macrophage polarization in an MR1-dependent manner and in the gut by inducing microbiota dysbiosis and loss of gut integrity. Both MAIT cell-induced tissue alterations contribute to metabolic dysfunction. Treatment with MAIT cell inhibitory ligand demonstrates its potential as a strategy against inflammation, dysbiosis and metabolic disorders. Inflammation, immune cells and the host microbiota are intimately linked in the pathophysiology of obesity and diabetes. Here the authors show mucosal-associated invariant T cells fuel inflammation in the tissues and serve a function in promoting metabolic breakdown, polarising macrophage populations and inducing dysbiosis of the intestinal microbiota. [ABSTRACT FROM AUTHOR]

Published

2020

8. Tumor invasion in draining lymph nodes is associated with Treg accumulation in breast cancer patients.

Author

Núñez, Nicolas Gonzalo, Tosello Boari, Jimena, Ramos, Rodrigo Nalio, Richer, Wilfrid, Cagnard, Nicolas, Anderfuhren, Cyrill Dimitri, Niborski, Leticia Laura, Bigot, Jeremy, Meseure, Didier, De La Rochere, Philippe, Milder, Maud, Viel, Sophie, Loirat, Delphine, Pérol, Louis, Vincent-Salomon, Anne, Sastre-Garau, Xavier, Burkhard, Becher, Sedlik, Christine, Lantz, Olivier, and Amigorena, Sebastian

Subjects

LYMPH nodes, CANCER patients, SUPPRESSOR cells, BREAST cancer, METASTATIC breast cancer

Abstract

Tumor-draining lymph node (TDLN) invasion by metastatic cells in breast cancer correlates with poor prognosis and is associated with local immunosuppression, which can be partly mediated by regulatory T cells (Tregs). Here, we study Tregs from matched tumor-invaded and non-invaded TDLNs, and breast tumors. We observe that Treg frequencies increase with nodal invasion, and that Tregs express higher levels of co-inhibitory/stimulatory receptors than effector cells. Also, while Tregs show conserved suppressive function in TDLN and tumor, conventional T cells (Tconvs) in TDLNs proliferate and produce Th1-inflammatory cytokines, but are dysfunctional in the tumor. We describe a common transcriptomic signature shared by Tregs from tumors and nodes, including CD80, which is significantly associated with poor patient survival. TCR RNA-sequencing analysis indicates trafficking between TDLNs and tumors and ongoing Tconv/Treg conversion. Overall, TDLN Tregs are functional and express a distinct pattern of druggable co-receptors, highlighting their potential as targets for cancer immunotherapy. Tumor-draining lymph nodes are often the first site of metastasis in breast cancer patients. Here, the authors show that metastatic lymph nodes are characterized by the accumulation of suppressive regulatory T cells with a distinct phenotype compared to matched non-invaded lymph nodes and tumors. [ABSTRACT FROM AUTHOR]

Published

2020

9. Induction of anergic or regulatory tumor-specific CD4+ T cells in the tumor-draining lymph node.

Author

Alonso, Ruby, Flament, Héloïse, Lemoine, Sébastien, Sedlik, Christine, Bottasso, Emanuel, Péguillet, Isabel, Prémel, Virginie, Denizeau, Jordan, Salou, Marion, Darbois, Aurélie, Gonzalo Núñez, Nicolás, Salomon, Benoit, Gross, David, Piaggio, Eliane, and Lantz, Olivier

Abstract

CD4+ T cell antitumor responses have mostly been studied in transplanted tumors expressing secreted model antigens (Ags), while most mutated proteins in human cancers are not secreted. The fate of Ag-specific CD4+ T cells recognizing a cytoplasmic Ag in mice bearing autochthonous tumors is still unclear. Here we show, using a genetically engineered lung adenocarcinoma mouse model, that naive tumor-specific CD4+ T cells are activated and proliferate in the tumor-draining lymph node (TdLN) but do not differentiate into effectors or accumulate in tumors. Instead, these CD4+ T cells are driven toward anergy or peripherally-induced Treg (pTreg) differentiation, from the early stage of tumor development. This bias toward immune suppression is restricted to the TdLN, and is maintained by Tregs enriched in the tumor Ag-specific cell population. Thus, tumors may enforce a dominant inhibition of the anti-tumor CD4 response in the TdLN by recapitulating peripheral self-tolerance mechanisms. [ABSTRACT FROM AUTHOR]

Published

2018

10. MAIT, MR1, microbes and riboflavin: a paradigm for the co-evolution of invariant TCRs and restricting MHCI-like molecules?

Author

Mondot, Stanislas, Boudinot, Pierre, and Lantz, Olivier

Subjects

MAJOR histocompatibility complex, T cell receptors, VITAMIN B2, MUCOUS membranes, MICROORGANISMS

Abstract

MAIT cells express an invariant TCR that recognizes non-peptidic microbial antigens presented by the non-polymorphic MHCI-like molecule, MR1. We briefly describe how the antigens recognized by MAIT cells are generated from an unstable precursor of the riboflavin (Vitamin B2) biosynthesis pathway, as well as the main features of MAIT cells in comparison with other related T cell subsets. In silico analysis of bacterial genomes shows that the riboflavin biosynthesis pathway is highly prevalent in all groups of Prokaryotes with, however, notable exceptions. We discuss the putative functions and the evolution of the MAIT/MR1 couple: it appeared in the ancestors of mammals and is highly conserved across this group, but was independently lost in three orders. We describe the four instances of known invariant TCR and MHC-I-like molecules encountered in Vertebrates. Both T cells bearing semi-invariant TCR and the associated, evolutionarily conserved MHC-I related molecules have been found in mammals or in amphibians, which suggests that other MHC1-like/invariant TCR couples might be present in other classes of Vertebrates to detect generic microbial compounds. This allows us to discuss how the recognition of riboflavin precursor derivatives by the MAIT TCR may be a way to detect invasive microbes in specific organs, and may epitomize other invariant T cell systems across vertebrates. [ABSTRACT FROM AUTHOR]

Published

2016

11. Upcoming translational challenges for uveal melanoma.

Author

Nabil, Amirouchene-Angelozzi, Marie, Schoumacher, Marc-Henri, Stern, Nathalie, Cassoux, Laurence, Desjardins, Sophie, Piperno-Neumann, Olivier, Lantz, Sergio, Roman-Roman, Amirouchene-Angelozzi, Nabil, Schoumacher, Marie, Stern, Marc-Henri, Cassoux, Nathalie, Desjardins, Laurence, Piperno-Neumann, Sophie, Lantz, Olivier, and Roman-Roman, Sergio

Subjects

ANIMALS, MELANOMA, GENETIC mutation, UVEA, TUMORS

Abstract

The past few years have witnessed major advances in the understanding of the molecular landscape of uveal melanoma (UM). The discovery of a mutational background that is completely different from the one of skin melanoma has granted to UM a stand-alone status. The absence of effective therapy for metastatic disease offers now a chessboard for targeted therapy but at the same time urges preclinical science to develop accordingly, to guide the use of economical resources to the best profit of patients. This review describes the current knowledge on the biology of this disease and discusses the challenges that must be undertaken to translate this knowledge into real benefit for patients. [ABSTRACT FROM AUTHOR]

Published

2015

12. Specific MAIT cell behaviour among innate-like T lymphocytes in critically ill patients with severe infections.

Author

Grimaldi, David, Bourhis, Lionel, Sauneuf, Bertrand, Dechartres, Agnès, Rousseau, Christophe, Ouaaz, Fatah, Milder, Maud, Louis, Delphine, Chiche, Jean-Daniel, Mira, Jean-Paul, Lantz, Olivier, and Pène, Frédéric

Subjects

T cells, INTENSIVE care units, LYMPHOCYTES, SEPSIS, BACTERIAL diseases

Abstract

Purpose: In between innate and adaptive immunity, the recently identified innate-like mucosal-associated invariant T (MAIT) lymphocytes display specific reactivity to non-streptococcal bacteria. Whether they are involved in bacterial sepsis has not been investigated. We aimed to assess the number and the time course of circulating innate-like T lymphocytes (MAIT, NKT and γδ T cells) in critically ill septic and non-septic patients and to establish correlations with the further development of intensive care unit (ICU)-acquired infections. Methods: We prospectively enrolled consecutive patients with severe sepsis and septic shock. Controls were critically ill patients with non-septic shock and age-matched healthy subjects. Circulating innate-like lymphocytes were enumerated using a flow cytometry assay at day 1, 4 and 7. Results: One hundred and fifty six patients (113 severe bacterial infections, 36 non-infected patients and 7 patients with severe viral infections) and 26 healthy subjects were enrolled into the study. Patients with severe bacterial infections displayed an early decrease in MAIT cell count [median 1.3/mm; interquartile range (0.4-3.2)] as compared to control healthy subjects [31.1/mm (12.1-45.2)], but also to non-infected critically ill patients [4.3/mm (1.4-13.2)] ( P < 0.0001 for all comparisons). In contrast NKT and γδ T cell counts did not differ between patients groups. The multivariate analysis identified non-streptococcal bacterial infection as an independent determinant of decrease in MAIT cell count. Furthermore, the incidence of ICU-acquired infections was higher in patients with persistent MAIT cell depletion. Conclusions: This large human study provides valuable information about MAIT cells in severe bacterial infections. The persistent depletion of MAIT cells is associated with the further development of ICU-acquired infections. [ABSTRACT FROM AUTHOR]

Published

2014

13. Proportions of CD4+ memory T cells are altered in individuals chronically infected with Schistosoma haematobium.

Author

Nausch, Norman, Bourke, Claire D., Appleby, Laura J., Rujeni, Nadine, Lantz, Olivier, Trottein, François, Midzi, Nicholas, Mduluza, Takafira, and Mutapi, Francisca

Abstract

Characterisation of protective helminth acquired immunity in humans or experimental models has focused on effector responses with little work conducted on memory responses. Here we show for the first time, that human helminth infection is associated with altered proportions of the CD4+ memory T cells, with an associated alteration of TH1 responses. The reduced CD4+ memory T cell proportions are associated with a significantly lower ratio of schistosome-specific IgE/IgG4 (marker for resistance to infection/re-infection) in uninfected older people. Helminth infection does not affect the CD8+ memory T cell pool. Furthermore, we show for the first time in a helminth infection that the CD4+ memory T cell proportions decline following curative anti-helminthic treatment despite increased CD4+ memory cell replication. Reduced accumulation of the CD4+ memory T cells in schistosome-infected people has implications for the development of natural or vaccine induced schistosome-specific protective immunity as well as for unrelated pathogens. [ABSTRACT FROM AUTHOR]

Published

2012

14. Quantifying Amplicons with ELISA.

Author

Walker, John M., Kochanowski, Bernd, Reischl, Udo, Lantz, Olivier, Bonney, Elizabeth, and Taoufik, Yassine

Abstract

Among the numerous assays proposed for quantifying specific nucleic-acid sequences in biological samples, PCR offers the greatest sensitivity and versatility. The assay for quantifying the amount of polymerase chain reaction (PCR) products is a crucial step in any quantitative PCR method. It should be sensitive and specific, able to display a wide dynamic range, nonradioactive, easy to do, and inexpensive. The results of the assay should also be easily digitalized. Quantification of amplicons with enzyme-linked immunosorbent assay (ELISA) fulfills these criteria. It can be automatized and readers are already available in most research and clinical laboratories. This assay can be accomplished by using colorimetry, fluorometry, or luminometry, depending on the substrate used. Luminometry displays the best sensitivity and has the widest dynamic range of these three methods (1 and see Subheading 1.2.3.). In this chapter, we will describe some of the available formats, the one we have been using this past few years, and its use in kinetic quantitative PCR or with internal standard. [ABSTRACT FROM AUTHOR]

Published

1999

15. Kinetic Quantitative PCR vs End-Point Quantitative PCR with Internal Standard.

Author

Walker, John M., Kochanowski, Bernd, Reischl, Udo, Lantz, Olivier, Bonney, Elizabeth, Griscelli, Franck, and Taoufik, Yassine

Abstract

Quantitative PCR can be done either by measuring the amount of PCR products at a given number of cycle (end-point quantitative PCR) (1-4) or by following the amount of products during the PCR at several cycles (kinetic quantitative PCR) (5,6). In this chapter, we define these two quantitative PCR methods, give their main characteristics, and compare their advantages and drawbacks. We then give a few examples of applications of the kinetic PCR method we have been using during the past few years. [ABSTRACT FROM AUTHOR]

Published

1999

16. Antimicrobial activity of mucosal-associated invariant T cells.

Author

Le Bourhis, Lionel, Martin, Emmanuel, Péguillet, Isabelle, Guihot, Amélie, Froux, Nathalie, Coré, Maxime, Lévy, Eva, Dusseaux, Mathilde, Meyssonnier, Vanina, Premel, Virginie, Ngo, Charlotte, Riteau, Béatrice, Duban, Livine, Robert, Delphine, Rottman, Martin, Soudais, Claire, and Lantz, Olivier

Subjects

T cells, MAJOR histocompatibility complex, LABORATORY mice, ANTI-infective agents, LIGANDS (Biochemistry), MYCOBACTERIUM

Abstract

Mucosal-associated invariant T lymphocytes (MAIT lymphocytes) are characterized by two evolutionarily conserved features: an invariant T cell antigen receptor (TCR) α-chain and restriction by the major histocompatibility complex (MHC)-related protein MR1. Here we show that MAIT cells were activated by cells infected with various strains of bacteria and yeast, but not cells infected with virus, in both humans and mice. This activation required cognate interaction between the invariant TCR and MR1, which can present a bacteria-derived ligand. In humans, we observed considerably fewer MAIT cells in blood from patients with bacterial infections such as tuberculosis. In the mouse, MAIT cells protected against infection by Mycobacterium abscessus or Escherichia coli. Thus, MAIT cells are evolutionarily conserved innate-like lymphocytes that sense and help fight off microbial infection. [ABSTRACT FROM AUTHOR]

Published

2010

17. Selection of evolutionarily conserved mucosal-associated invariant T cells by MR1.

Author

Treiner, Emmanuel, Duban, Livine, Bahram, Seiamak, Radosavljevic, Mirjana, Wanner, Valerie, Tilloy, Florence, Affaticati, Pierre, Gilfillan, Susan, and Lantz, Olivier

Subjects

T cells, KILLER cells, MAJOR histocompatibility complex

Abstract

The evolutionary conservation of T lymphocyte subsets bearing T-cell receptors (TCRs) using invariant α-chains is indicative of unique functions. CD1d-restricted natural killer T (NK-T) cells that express an invariant Vα14TCRα chain have been implicated in microbial and tumour responses, as well as in auto-immunity. Here we show that T cells that express the canonical hVα7.2-Jα33 or mVα19-Jα33 TCR rearrangement are preferentially located in the gut lamina propria of humans and mice, respectively, and are therefore genuine mucosal-associated invariant T (MAIT) cells. Selection and/or expansion of this population requires B lymphocytes, as MAIT cells are absent in B-cell-deficient patients and mice. In addition, we show that MAIT cells are selected and/or restricted by MR1, a monomorphic major histocompatibility complex class I-related molecule that is markedly conserved in diverse mammalian species. MAIT cells are not present in germfree mice, indicating that commensal flora is required for their expansion in the gut lamina propria. This indicates that MAIT cells are probably involved in the host response at the site of pathogen entry, and may regulate intestinal B-cell activity. [ABSTRACT FROM AUTHOR]

Published

2003

18. Indirect activation of naïve CD4+ T cells by dendritic cell–derived exosomes.

Author

Théry, Clotilde, Duban, Livine, Segura, Elodie, Véron, Philippe, Lantz, Olivier, and Amigorena, Sebastian

Subjects

DENDRITIC cells, MAJOR histocompatibility complex, T cells

Abstract

Dendritic cells (DCs) secrete vesicles of endosomal origin, called exosomes, that bear major histocompatibility complex (MHC) and T cell costimulatory molecules. Here, we found that injection of antigen- or peptide-bearing exosomes induced antigen-specific naive CD4[sup +] T cell activation in vivo. In vitro, exosomes did not induce antigen-dependent T cell stimulation unless mature CD8α-DCs were also present in the cultures. These mature DCs could be MHC class II-negative, but had to bear CD80 and CD86. Therefore, in addition to carrying antigen, exosomes promote the exchange of functional peptide-MHC complexes between DCs. Such a mechanism may increase the number of DCs bearing a particular peptide, thus amplifying the initiation of primary adaptive immune responses. [ABSTRACT FROM AUTHOR]

Published

2002

19. Cross-primed CD8+ T cells mediate graft rejection via a distinct effector pathway.

Author

Valujskikh, Anna, Lantz, Olivier, Celli, Susanna, Matzinger, Polly, and Heeger, Peter S.

Subjects

*GRAFT rejection, *T cells

Abstract

To prevent bystander destruction of healthy host tissues, cytotoxic CD8[SUP+] T lymphocytes are fitted with specific receptors that direct their destructive forces specifically against chosen targets. We show here, however, that anti-H-Y monospecific, H-2[SUPb]-restricted MataHari CD8[SUP+] T cells reject H-2[SUPk] male skin grafts, with which they cannot directly interact. Such rejection is interferon-γ-dependent and only occurs if the recipient endothelium expresses H-2[SUPb]. The findings suggest an alternate indirect effector pathway that requires processing and presentation of the donor H-Y antigen by recipient endothelium and have implications for both transplantation and autoimmune disease. [ABSTRACT FROM AUTHOR]

Published

2002

20. γ chain required for naïve CD4+ T cell survival but not for antigen proliferation.

Author

Lantz, Olivier, Grandjean, Isabelle, Matzinger, Polly, and Di Santo, James P.

Subjects

*HOMEOSTASIS, *IMMUNODEFICIENCY, *T cells, *IMMUNE system

Abstract

Lymphoid homeostasis is required to ensure immune responsiveness and to prevent immunodeficiency. As such, the immune system must maintain distinct populations of naïve T cells that are able to respond to new antigens as well as memory T cells specific to those antigens it has already encountered. Though both naïve and memory T cells reside in and traffic through secondary lymphoid organs, there is growing evidence that the two populations may be regulated differently. We show here that naïve T cell survival and memory T cell survival have different requirements for cytokines (including the interleukins IL-2, IL-4, IL-7, IL-9 and IL-15) that use the common cytokine receptor gamma chain (γc). Using monoclonal populations of antigen-specific CD4+ T cells, we found that naïve T cells cannot survive without γc, whereas memory T cells show no such requirement. In contrast, neither naïve nor γc-deficient memory T cells were impaired in their ability to proliferate and produce cytokines in response to in vivo antigenic stimulation. These data call into question the physiological role of γc-dependent cytokines as T cell growth factors and show that naïve and memory CD4+ T cell survival is maintained by distinct mechanisms. [ABSTRACT FROM AUTHOR]

Published

2000

21. Upcoming translational challenges for uveal melanoma.

Author

Amirouchene-Angelozzi, Nabil, Schoumacher, Marie, Stern, Marc-Henri, Cassoux, Nathalie, Desjardins, Laurence, Piperno-Neumann, Sophie, Lantz, Olivier, and Roman-Roman, Sergio

Published

2015

22. Corrigendum: Antimicrobial activity of mucosal-associated invariant T cells.

Author

Le Bourhis, Lionel, Martin, Emmanuel, Péguillet, Isabelle, Guihot, Amélie, Froux, Nathalie, Coré, Maxime, Lévy, Eva, Dusseaux, Mathilde, Meyssonnier, Vanina, Premel, Virginie, Ngo, Charlotte, Riteau, Béatrice, Duban, Livine, Robert, Delphine, Rottman, Martin, Soudais, Claire, and Lantz, Olivier

Subjects

AUTHORS

Abstract

A correction to the article "Antimicrobial activity of mucosal-associated invariant T cells" that was published online in the June 27,2010 issue is presented.

Published

2010

23. corrigendum: Selection of evolutionarily conserved mucosal-associated invariant T cells by MR1.

Author

Treiner, Emmanuel, Duban, Livine, Bahram, Seiamak, Radosavljevic, Mirjana, Wanner, Valerie, Tilloy, Florence, Affaticati, Pierre, Gilfillan, Susan, and Lantz, Olivier

Subjects

PERIODICALS, EXPERIENTIAL research

Abstract

Presents an addendum to an article 'Non-Classical Receptive Field Mediates Switch in a Sensory Neuron's Frequency Tuning,' which appeared in an earlier issue of the magazine 'Nature.'

Published

2003