Your search keyword '"Luce, Sandrine"' showing total 5 results

1. Preclinical Models to Evaluate the Human Response to Autoantigen and Antigen-Specific Immunotherapy in Human Type 1 Diabetes.

Author

Houeiss, Pamela, Boitard, Christian, and Luce, Sandrine

Subjects

TYPE 1 diabetes, ANIMAL models in research, AUTOIMMUNE diseases, IMMUNOLOGICAL tolerance, T cells, TRANSGENIC mice

Abstract

Type 1 Diabetes (T1D) is an autoimmune disease that results from the destruction of pancreatic islet β-cells by auto-reactive T cells. The clinical management of T1D faces the lack of fully predictive biomarkers in its preclinical stage and of antigen-specific therapies to induce or re-induce immune tolerance to β-cell autoantigens and prevent its development. From a therapeutic standpoint, preclinical models of T1D have fallen short of directly translating into humans. To circumvent this limitation, preclinical models are being optimized to allow defining autoantigen epitopes that are presented to T cells and directly apply to the human. In this review, we propose to make a point on the latest available models such as humanized immunodeficient NOD mice models and HLA and autoantigen transgenic mice and their application in the context of T1D. [ABSTRACT FROM AUTHOR]

Published

2022

2. A Humanized Mouse Strain That Develops Spontaneously Immune-Mediated Diabetes.

Author

Luce, Sandrine, Guinoiseau, Sophie, Gadault, Alexis, Letourneur, Franck, Nitschke, Patrick, Bras, Marc, Vidaud, Michel, Charneau, Pierre, Larger, Etienne, Colli, Maikel L., Eizirik, Decio L., Lemonnier, François, and Boitard, Christian

Subjects

TYPE 1 diabetes, PANCREATIC beta cells, MAJOR histocompatibility complex, TYPE 2 diabetes, HISTOCOMPATIBILITY antigens, MICE, T cells, HISTOCOMPATIBILITY class I antigens, AUTOIMMUNE diseases

Abstract

To circumvent the limitations of available preclinical models for the study of type 1 diabetes (T1D), we developed a new humanized model, the YES-RIP-hB7.1 mouse. This mouse is deficient of murine major histocompatibility complex class I and class II, the murine insulin genes, and expresses as transgenes the HLA-A*02:01 allele, the diabetes high-susceptibility HLA-DQ8A and B alleles, the human insulin gene, and the human co-stimulatory molecule B7.1 in insulin-secreting cells. It develops spontaneous T1D along with CD4+ and CD8+ T-cell responses to human preproinsulin epitopes. Most of the responses identified in these mice were validated in T1D patients. This model is amenable to characterization of hPPI-specific epitopes involved in T1D and to the identification of factors that may trigger autoimmune response to insulin-secreting cells in human T1D. It will allow evaluating peptide-based immunotherapy that may directly apply to T1D in human and complete preclinical model availability to address the issue of clinical heterogeneity of human disease. [ABSTRACT FROM AUTHOR]

Published

2021

3. Humanized Mouse Model to Study Type 1 Diabetes.

Author

Luce, Sandrine, Guinoiseau, Sophie, Gadault, Alexis, Letourneur, Franck, Blondeau, Bertrand, Nitschke, Patrick, Pasmant, Eric, Vidaud, Michel, Lemonnier, François, and Boitard, Christian

Subjects

*TYPE 1 diabetes, *PANCREATIC beta cells, *LABORATORY mice, *T cells, *GENOTYPES, *IMMUNE response, *AGING, *ANIMAL experimentation, *AUTOIMMUNE diseases, *BIOLOGICAL models, *COMPARATIVE studies, *GENETIC techniques, *IMMUNITY, *INSULIN, *ISLANDS of Langerhans, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *NUCLEOTIDES, *PREDIABETIC state, *PROTEIN precursors, *RESEARCH, *HLA-B27 antigen, *EVALUATION research, *DISEASE progression

Abstract

Key requirements in type 1 diabetes (T1D) are in setting up new assays as diagnostic biomarkers that will apply to prediabetes, likely T-cell assays, and in designing antigen-specific therapies to prevent T1D development. New preclinical models of T1D will be required to help with advancing both aims. By crossing mouse strains that lack either murine MHC class I and class II genes and insulin genes, we developed YES mice that instead express human HLA-A*02:01, HLA-DQ8, and insulin genes as transgenes. The metabolic and immune phenotype of YES mice is basically identical to that of the parental strains. YES mice remain insulitis and diabetes free up to 1 year of follow-up, maintain normoglycemia to an intraperitoneal glucose challenge in the long-term range, have a normal β-cell mass, and show normal immune responses to conventional antigens. This new model has been designed to evaluate adaptive immune responses to human insulin on a genetic background that recapitulates a human high-susceptibility HLA-DQ8 genetic background. Although insulitis free, YES mice develop T1D when challenged with polyinosinic-polycytidylic acid. They allow the characterization of preproinsulin epitopes recognized by CD8+ and CD4+ T cells upon immunization against human preproinsulin or during diabetes development. [ABSTRACT FROM AUTHOR]

Published

2018

4. Potential Role of IL-17-Producing iNKT Cells in Type 1 Diabetes.

Author

Li, Shamin, Joseph, Claudine, Becourt, Chantal, Klibi, Jihene, Luce, Sandrine, Dubois-Laforgue, Daniele, Larger, Etienne, Boitard, Christian, and Benlagha, Kamel

Subjects

INTERLEUKIN-17, KILLER cells, TYPE 1 diabetes, AUTOIMMUNE diseases, CYTOKINES, BLOOD cells, IMMUNE system

Abstract

We explored in this study the status and potential role of IL-17-producing iNKT cells (iNKT17) in type 1 diabetes (T1D) by analyzing these cells in patients with T1D, and in NOD mice, a mouse model for T1D. Our analysis in mice showed an increase of iNKT17 cells in NOD vs control C57BL/6 mice, partly due to a better survival of these cells in the periphery. We also found a higher frequency of these cells in autoimmune-targeted organs with the occurrence of diabetes, suggesting their implication in the disease development. In humans, though absent in fresh PMBCs, iNKT17 cells are detected in vitro with a higher frequency in T1D patients compared to control subjects in the presence of the proinflammatory cytokine IL-1β, known to contribute to diabetes occurrence. These IL-1β-stimulated iNKT cells from T1D patients keep their potential to produce IFN-γ, a cytokine that drives islet β-cell destruction, but not IL-4, with a reverse picture observed in healthy volunteers. On the whole, our results argue in favour of a potential role of IL-17-producing iNKT cells in T1D and suggest that inflammation in T1D patients could induce a Th1/Th17 cytokine secretion profile in iNKT cells promoting disease development. [ABSTRACT FROM AUTHOR]

Published

2014

5. Recognition of Human Proinsulin Leader Sequence by Class I--Restricted T-Cells in HLA-A*0201 Transgenic Mice and in Human Type 1 Diabetes.

Author

Toma, Andréa, Laïka, Taghrid, Haddouk, Samy, Luce, Sandrine, Briand, Jean-Paul, Camoin, Luc, Connan, Francine, Lambert, Marion, Caillat-Zucman, Sophie, Carel, Jean-Claude, Muller, Sylviane, Choppin, Jeannine, Lemonnier, Francois, and Boitard, Christian

Subjects

PROINSULIN, T cells, HLA histocompatibility antigens, TRANSGENIC mice, DIABETES

Abstract

OBJECTIVE--A restricted region of proinsulin located in the B chain and adjacent region of C-peptide has been shown to contain numerous candidate epitopes recognized by CD8[sup +] T-cells. Our objective is to characterize HLA class I-restricted epitopes located within the preproinsulin leader sequence. RESEARCH DESIGN AND METHODS--Seven 8- to 11-mer preproinsulin peptides carrying anchoring residues for HLA-A1, -A2, -A24, and -B8 were selected from databases. HLA-A2-restricted peptides were tested for immunogenicity in transgenic mice expressing a chimeric HLA-A*0201/β2-microglobulin molecule. The peptides were studied for binding to purified HLA class I molecules, selected for carrying COOH-terminal residues generated by proteasome digestion in vitro and tested for recognition by human lymphocytes using an ex vivo interferon-γ (IFN-γ) ELISpot assay. RESULTS--Five HLA-A2-restricted peptides were immunogenic in transgenic mice. Murine T-cell clones specific for these peptides were cytotoxic against cells transfected with the preproinsulin gene. They were recognized by peripheral blood mononuclear cells (PBMCs) from 17 of 21 HLA-A2 type 1 diabetic patients. PBMCs from 25 of 38 HLA-A1, -A2, -A24, or -B8 patients produced IFN-γ in response to six preproinsulin peptides covering residues 2-25 within the preproinsulin region. In most patients, the response was against several class I--restricted peptides. T-cells recognizing preproinsulin peptide were characterized as CD8[sup +] T-cells by staining with peptide/ HLA-A2 tetramers. CONCLUSIONS--We defined class I-restricted epitopes located within the leader sequence of human preproinsulin through in vivo (transgenic mice) and ex vivo (diabetic patients) assays, illustrating the possible role of preproinsulin-specific CD8[sup +] T-cells in human type 1 diabetes. Diabetes 58:394-402, 2009 [ABSTRACT FROM AUTHOR]

Published

2009