Your search keyword '"Paula Tomas Ojer"' showing total 14 results

1. Characterization of Antigen-Induced CD4+ T-Cell Senescence in Multiple Sclerosis

Author

Paula Tomas-Ojer, Marco Puthenparampil, Carolina Cruciani, María José Docampo, Roland Martin, and Mireia Sospedra

Subjects

multiple sclerosis (MS), CD4, T-cell, T-cell senescence, regulation, Neurology. Diseases of the nervous system, RC346-429

Abstract

Antigen-induced T-cell exhaustion and T-cell senescence are peripheral regulatory mechanisms that control effector T-cell responses. Markers of exhaustion and senescence on T Cells indicate the previous activation by repetitive stimulation with specific antigens. Malignant tumors are accompanied by enhanced T-cell exhaustion and T-cell senescence resulting in immune evasion, while these control mechanisms might be diminished in autoimmune diseases including multiple sclerosis (MS). To better understand the involvement of antigen-induced T-cell senescence in controlling CD4+ T-cell-mediated autoimmune responses in MS, we have analyzed the re-expression of CD45RA and the downregulation of CD28 and CD27 molecules as markers of antigen-induced T-cell senescence in fresh cerebrospinal fluid (CSF)-infiltrating and paired circulating T cells from patients with MS. Patients with different levels of CD4+ T-cell senescence were identified and characterized regarding demographical and clinical features as well as intrathecal markers of neurodegeneration. CD4+ T-cell senescence was also analyzed in control patients to explore a putative deficit of this regulatory mechanism in MS. This study shows heterogeneity of markers of CD4+ T-cell senescence in patients with MS. Patients with high levels of CD4+ T-cell senescence in peripheral blood showed increased frequencies of CSF-infiltrating CD28+ CD27-EM CD4+ T cells with a proinflammatory Th1 functional phenotype. The correlation of these cells with the intrathecal levels of neurofilament light chain, a marker of neurodegeneration, suggests their relevance in disease pathogenesis and the involvement of T-cell senescence in their regulation. Markers of antigen-induced T-senescence, therefore, show promise as a tool to identify pathogenic CD4+ T cells in patients with MS.

Published

2022

2. Brain Citrullination Patterns and T Cell Reactivity of Cerebrospinal Fluid-Derived CD4+ T Cells in Multiple Sclerosis

Author

Wolfgang Faigle, Carolina Cruciani, Witold Wolski, Bernd Roschitzki, Marco Puthenparampil, Paula Tomas-Ojer, Carla Sellés-Moreno, Thomas Zeis, Ivan Jelcic, Nicole Schaeren-Wiemers, Mireia Sospedra, and Roland Martin

Subjects

human brain, multiple sclerosis, citrullination, T cell reactivity, autoimmune, proteomics, Immunologic diseases. Allergy, RC581-607

Abstract

Immune responses to citrullinated peptides have been described in autoimmune diseases like rheumatoid arthritis (RA) and multiple sclerosis (MS). We investigated the post-translational modification (PTM), arginine to citrulline, in brain tissue of MS patients and controls (C) by proteomics and subsequently the cellular immune response of cerebrospinal fluid (CSF)-infiltrating T cells to citrullinated and unmodified peptides of myelin basic protein (MBP). Using specifically adapted tissue extraction- and combined data interpretation protocols we could establish a map of citrullinated proteins by identifying more than 80 proteins with two or more citrullinated peptides in human brain tissue. We report many of them for the first time. For the already described citrullinated proteins MBP, GFAP, and vimentin, we could identify additional citrullinated sites. The number of modified proteins in MS white matter was higher than control tissue. Citrullinated peptides are considered neoepitopes that may trigger autoreactivity. We used newly identified epitopes and previously reported immunodominant myelin peptides in their citrullinated and non-citrullinated form to address the recognition of CSF-infiltrating CD4+ T cells from 22 MS patients by measuring proliferation and IFN-γ secretion. We did not detect marked responses to citrullinated peptides, but slightly more strongly to the non-modified version. Based on these data, we conclude that citrullination does not appear to be an important activating factor of a T cell response, but could be the consequence of an immune- or inflammatory response. Our approach allowed us to perform a deep proteome analysis and opens new technical possibilities to analyze complex PTM patterns on minute quantities of rare tissue samples.

Published

2019

3. Figure S7 from Vaccination with Designed Neopeptides Induces Intratumoral, Cross-reactive CD4+ T-cell Responses in Glioblastoma

Author

Roland Martin, Patrick Roth, Michael Weller, Luca Regli, Bernd Bodenmiller, Erich F. Greiner, Holger Moch, Mireia Sospedra, Andreas Lutterotti, Catherine J. Wu, Ron McKay, Joo Heon Shin, Barbara Schrörs, Susanne Dettwiler, Elisabeth Rushing, Daniel Schulz, Ivan Jelcic, Gioele Medici, Paula Tomas Ojer, Magdalena Foege, Carla Sellés Moreno, Reza Naghavian, Nora C. Toussaint, Marian C. Neidert, Tobias Weiss, and Jian Wang

Abstract

Designed mutations increase the stimulatory strength of D-neopeptides above N-peptides. (A) TILs were stimulated with 5 μM class I-peptides, including N-peptides and D-neopeptides, for 5 days. 5 replicate wells were tested for proliferation, and proliferation was measured by 3H-thymidine incorporation assay. In each group, the N-peptides and their corresponding D-neopeptides are included, and the designed mutated positions are highlighted in the red box. The blue dotted line indicates the mean value of the no peptide control. The red dotted line indicates the mean value plus three standard deviations of the no peptide control. Values above the red dotted line were considered positive. (#) indicates the peptide that was used in the 1st to 4th vaccinations. (B) TILs were stimulated with 5 μM class II-peptides, including N-peptides and D-neopeptides, for 5 days. 5 replicate wells were tested for proliferation, and proliferation was measured by 3H-thymidine incorporation assay.

Published

2023

4. Table S4 from Vaccination with Designed Neopeptides Induces Intratumoral, Cross-reactive CD4+ T-cell Responses in Glioblastoma

Author

Roland Martin, Patrick Roth, Michael Weller, Luca Regli, Bernd Bodenmiller, Erich F. Greiner, Holger Moch, Mireia Sospedra, Andreas Lutterotti, Catherine J. Wu, Ron McKay, Joo Heon Shin, Barbara Schrörs, Susanne Dettwiler, Elisabeth Rushing, Daniel Schulz, Ivan Jelcic, Gioele Medici, Paula Tomas Ojer, Magdalena Foege, Carla Sellés Moreno, Reza Naghavian, Nora C. Toussaint, Marian C. Neidert, Tobias Weiss, and Jian Wang

Abstract

Predicted TSA/TAA-derived N-peptides and D-neopeptides

Published

2023

5. Data from Vaccination with Designed Neopeptides Induces Intratumoral, Cross-reactive CD4+ T-cell Responses in Glioblastoma

Author

Roland Martin, Patrick Roth, Michael Weller, Luca Regli, Bernd Bodenmiller, Erich F. Greiner, Holger Moch, Mireia Sospedra, Andreas Lutterotti, Catherine J. Wu, Ron McKay, Joo Heon Shin, Barbara Schrörs, Susanne Dettwiler, Elisabeth Rushing, Daniel Schulz, Ivan Jelcic, Gioele Medici, Paula Tomas Ojer, Magdalena Foege, Carla Sellés Moreno, Reza Naghavian, Nora C. Toussaint, Marian C. Neidert, Tobias Weiss, and Jian Wang

Abstract

Purpose:The low mutational load of some cancers is considered one reason for the difficulty to develop effective tumor vaccines. To overcome this problem, we developed a strategy to design neopeptides through single amino acid mutations to enhance their immunogenicity.Experimental Design:Exome and RNA sequencing as well as in silico HLA-binding predictions to autologous HLA molecules were used to identify candidate neopeptides. Subsequently, in silico HLA-anchor placements were used to deduce putative T-cell receptor (TCR) contacts of peptides. Single amino acids of TCR contacting residues were then mutated by amino acid replacements. Overall, 175 peptides were synthesized and sets of 25 each containing both peptides designed to bind to HLA class I and II molecules applied in the vaccination. Upon development of a tumor recurrence, the tumor-infiltrating lymphocytes (TIL) were characterized in detail both at the bulk and clonal level.Results:The immune response of peripheral blood T cells to vaccine peptides, including natural peptides and designed neopeptides, gradually increased with repetitive vaccination, but remained low. In contrast, at the time of tumor recurrence, CD8+ TILs and CD4+ TILs responded to 45% and 100%, respectively, of the vaccine peptides. Furthermore, TIL-derived CD4+ T-cell clones showed strong responses and tumor cell lysis not only against the designed neopeptide but also against the unmutated natural peptides of the tumor.Conclusions:Turning tumor self-peptides into foreign antigens by introduction of designed mutations is a promising strategy to induce strong intratumoral CD4+ T-cell responses in a cold tumor like glioblastoma.

Published

2023

6. Supplementary Tables 1, 3, 5-7 from Vaccination with Designed Neopeptides Induces Intratumoral, Cross-reactive CD4+ T-cell Responses in Glioblastoma

Author

Roland Martin, Patrick Roth, Michael Weller, Luca Regli, Bernd Bodenmiller, Erich F. Greiner, Holger Moch, Mireia Sospedra, Andreas Lutterotti, Catherine J. Wu, Ron McKay, Joo Heon Shin, Barbara Schrörs, Susanne Dettwiler, Elisabeth Rushing, Daniel Schulz, Ivan Jelcic, Gioele Medici, Paula Tomas Ojer, Magdalena Foege, Carla Sellés Moreno, Reza Naghavian, Nora C. Toussaint, Marian C. Neidert, Tobias Weiss, and Jian Wang

Abstract

Supplementary Table 1. Somatic mutations of the patient's glioblastoma; Supplementary Table 2. See Excel File; Supplementary Table 3. Literature-derived, glioblastoma-associated TAAs; Supplementary Table 4. See Excel File; Supplementary Table 5. Over-/highly expressed genes that were chosen for the design of vaccine peptides; Supplementary Table 6. Peptide cocktails for vaccination; Supplementary Table 7. Antibodies for imaging mass cytometry.

Published

2023

7. Vaccination with designed neopeptides induces intratumoral, cross-reactive CD4+ T cell responses in glioblastoma

Author

Jian Wang, Tobias Weiss, Marian C. Neidert, Nora C. Toussaint, Reza Naghavian, Carla Sellés Moreno, Magdalena Foege, Paula Tomas Ojer, Gioele Medici, Ivan Jelcic, Daniel Schulz, Elisabeth Rushing, Susanne Dettwiler, Barbara Schrörs, Joo Heon Shin, Ron McKay, Catherine J. Wu, Andreas Lutterotti, Mireia Sospedra, Holger Moch, Erich F. Greiner, Bernd Bodenmiller, Luca Regli, Michael Weller, Patrick Roth, Roland Martin, and University of Zurich

Subjects

Cancer Research, Oncology, 10049 Institute of Pathology and Molecular Pathology, 610 Medicine & health, 11493 Department of Quantitative Biomedicine, 10040 Clinic for Neurology

Abstract

Purpose: The low mutational load of some cancers is considered one reason for the difficulty to develop effective tumor vaccines. To overcome this problem, we developed a strategy to design neopeptides through single amino acid mutations to enhance their immunogenicity. Experimental Design: Exome and RNA sequencing as well as in silico HLA-binding predictions to autologous HLA molecules were used to identify candidate neopeptides. Subsequently, in silico HLA-anchor placements were used to deduce putative T-cell receptor (TCR) contacts of peptides. Single amino acids of TCR contacting residues were then mutated by amino acid replacements. Overall, 175 peptides were synthesized and sets of 25 each containing both peptides designed to bind to HLA class I and II molecules applied in the vaccination. Upon development of a tumor recurrence, the tumor-infiltrating lymphocytes (TIL) were characterized in detail both at the bulk and clonal level. Results: The immune response of peripheral blood T cells to vaccine peptides, including natural peptides and designed neopeptides, gradually increased with repetitive vaccination, but remained low. In contrast, at the time of tumor recurrence, CD8+ TILs and CD4+ TILs responded to 45% and 100%, respectively, of the vaccine peptides. Furthermore, TIL-derived CD4+ T-cell clones showed strong responses and tumor cell lysis not only against the designed neopeptide but also against the unmutated natural peptides of the tumor. Conclusions: Turning tumor self-peptides into foreign antigens by introduction of designed mutations is a promising strategy to induce strong intratumoral CD4+ T-cell responses in a cold tumor like glioblastoma., Clinical Cancer Research, 28 (24), ISSN:1078-0432, ISSN:1557-3265

Published

2022

8. Characterization of Antigen-Induced CD4+ T-Cell Senescence in Multiple Sclerosis

Author

Paula, Tomas-Ojer, Puthenparampil, Marco, Thorsten, Hornemann, Andreas, Lutterotti, Ilijas, Jelcic, Mario, Ziegler, Andreas, J Hülsmeier, Carolina, Cruciani, Wolfgang, Faigle, Roland, Martin, and Mireia, Sospedra.

Published

2022

9. Characterization of Antigen-Induced CD4+ T-Cell Senescence in Multiple Sclerosis

Author

Paula, Tomas-Ojer, Marco, Puthenparampil, Carolina, Cruciani, María José, Docampo, Roland, Martin, and Mireia, Sospedra

Abstract

Antigen-induced T-cell exhaustion and T-cell senescence are peripheral regulatory mechanisms that control effector T-cell responses. Markers of exhaustion and senescence on T Cells indicate the previous activation by repetitive stimulation with specific antigens. Malignant tumors are accompanied by enhanced T-cell exhaustion and T-cell senescence resulting in immune evasion, while these control mechanisms might be diminished in autoimmune diseases including multiple sclerosis (MS). To better understand the involvement of antigen-induced T-cell senescence in controlling CD4+ T-cell-mediated autoimmune responses in MS, we have analyzed the re-expression of CD45RA and the downregulation of CD28 and CD27 molecules as markers of antigen-induced T-cell senescence in fresh cerebrospinal fluid (CSF)-infiltrating and paired circulating T cells from patients with MS. Patients with different levels of CD4+ T-cell senescence were identified and characterized regarding demographical and clinical features as well as intrathecal markers of neurodegeneration. CD4+ T-cell senescence was also analyzed in control patients to explore a putative deficit of this regulatory mechanism in MS. This study shows heterogeneity of markers of CD4+ T-cell senescence in patients with MS. Patients with high levels of CD4+ T-cell senescence in peripheral blood showed increased frequencies of CSF-infiltrating CD28+ CD27-EM CD4+ T cells with a proinflammatory Th1 functional phenotype. The correlation of these cells with the intrathecal levels of neurofilament light chain, a marker of neurodegeneration, suggests their relevance in disease pathogenesis and the involvement of T-cell senescence in their regulation. Markers of antigen-induced T-senescence, therefore, show promise as a tool to identify pathogenic CD4+ T cells in patients with MS.

Published

2021

10. Altered CSF Albumin Quotient Links Peripheral Inflammation and Brain Damage in MS

Author

Marco Puthenparampil, Mireia Sospedra, Ilijas Jelcic, Andreas Lutterotti, Carolina Cruciani, Wolfgang Faigle, Andreas J. Hülsmeier, Mario Ziegler, Thorsten Hornemann, Paula Tomas-Ojer, Roland Martin, and University of Zurich

Subjects

Adult, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Multiple Sclerosis, Inflammation, 610 Medicine & health, Brain damage, Systemic inflammation, Article, CHI3L1, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Immunophenotyping, Albumins, 540 Chemistry, Humans, Medicine, CSF albumin, 10038 Institute of Clinical Chemistry, business.industry, Albumin, Middle Aged, 10040 Clinic for Neurology, 030104 developmental biology, 2728 Neurology (clinical), Neurology, Blood-Brain Barrier, Brain Injuries, Immunoglobulin G, 2808 Neurology, Female, Neurology (clinical), medicine.symptom, business, Biomarkers, 030217 neurology & neurosurgery

Abstract

ObjectiveCNS damage can increase the susceptibility of the blood-brain barrier (BBB) to changes induced by systemic inflammation. The aim of this study is to better understand BBB permeability in patients with MS and to examine whether compromised BBB integrity in some of these patients is associated with CNS damage and systemic inflammation.MethodsRoutine CSF measurements of 121 patients with MS were analyzed including number and type of infiltrating cells, total protein, lactate, and oligoclonal bands, as well as intrathecal production of immunoglobulins and CSF/serum quotients for albumin, immunoglobulins, and glucose. In addition, in a subcohort of these patients, we performed ex vivo immunophenotyping of CSF-infiltrating and paired circulating lymphocytes using a panel of 13 monoclonal antibodies, we quantified intrathecal neurofilament light chain (NF-L) and chitinase 3-like 1 (CHI3L1), and we performed intrathecal lipidomic analysis.ResultsPatients with MS with abnormal high levels of albumin in the CSF showed a distinct CSF cell infiltrate and markers of CNS damage such as increased intrathecal levels of NF-L and CHI3L1 as well as a distinct CSF lipidomic profile. In addition, these patients showed higher numbers of circulating proinflammatory Th1 and Th1* cells compatible with systemic inflammation. Of interest, the abnormally high levels of albumin in the CSF of those patients were preserved over time.ConclusionsOur results support the hypothesis that CNS damage may increase BBB vulnerability to systemic inflammation in a subset of patients and thus contribute to disease heterogeneity.

Published

2021

11. T-Cell Specificity Influences Disease Heterogeneity in Multiple Sclerosis

Author

Paula Tomas-Ojer, Mireia Sospedra, Roland Martin, Raquel Planas, Ivan Jelcic, Carla A. Wicki, Praveena Manogaran, Roland Opfer, Marco Puthenparampil, Ilijas Jelcic, Maria Jose Docampo, Carolina Cruciani, Markus Reindl, Andreas Lutterotti, and University of Zurich

Subjects

Adult, Male, Multiple Sclerosis, T-Lymphocytes, Clinical Neurology, 610 Medicine & health, T-Cell Antigen Receptor Specificity, Article, Myelin oligodendrocyte glycoprotein, Transcriptome, Myelin, Immunophenotyping, Antigen, medicine, Humans, Interferon gamma, Autoimmune disease, biology, business.industry, Multiple sclerosis, Middle Aged, medicine.disease, Magnetic Resonance Imaging, 10040 Clinic for Neurology, 2728 Neurology (clinical), medicine.anatomical_structure, Neurology, 2808 Neurology, Immunology, biology.protein, Female, Myelin-Oligodendrocyte Glycoprotein, Neurology (clinical), business, medicine.drug

Abstract

Background and Objectives Encouraged by the enormous progress that the identification of specific autoantigens added to the understanding of neurologic autoimmune diseases, we undertook here an in-depth study of T-cell specificities in the autoimmune disease multiple sclerosis (MS), for which the spectrum of responsible autoantigens is not fully defined yet. The identification of target antigens in MS is crucial for therapeutic strategies aimed to induce antigen-specific tolerance. In addition, knowledge of relevant T-cell targets can improve our understanding of disease heterogeneity, a hallmark of MS that complicates clinical management. Methods The proliferative response and interferon gamma (IFN-γ) release of CSF-infiltrating CD4+ T cells from patients with MS against several autoantigens was used to identify patients with different intrathecal T-cell specificities. Fresh CSF-infiltrating and paired circulating lymphocytes in these patients were characterized in depth by ex vivo immunophenotyping and transcriptome analysis of relevant T-cell subsets. Further examination of these patients included CSF markers of inflammation and neurodegeneration and a detailed characterization with respect to demographic, clinical, and MRI features. Results By testing CSF-infiltrating CD4+ T cells from 105 patients with MS against seven long-known myelin and five recently described GDP-l-fucose synthase peptides, we identified GDP-l-fucose synthase and myelin oligodendrocyte glycoprotein (35-55) responder patients. Immunophenotyping of CSF and paired blood samples in these patients revealed a significant expansion of an effector memory (CCR7− CD45RA−) CD27− Th1 CD4+ cell subset in GDP-l-fucose synthase responders. Subsequent transcriptome analysis of this subset demonstrated expression of Th1 and cytotoxicity-associated genes. Patients with different intrathecal T-cell specificities also differ regarding inflammation- and neurodegeneration-associated biomarkers, imaging findings, expression of HLA class II alleles, and seasonal distribution of the time of the lumbar puncture. Discussion Our observations reveal an association between autoantigen reactivity and features of disease heterogeneity that strongly supports an important role of T-cell specificity in MS pathogenesis. These data have the potential to improve patient classification in clinical practice and to guide the development of antigen-specific tolerization strategies., Neurology: Neuroimmunology & Neuroinflammation, 8 (6), ISSN:2332-7812

Published

2021

12. Brain Citrullination Patterns and T Cell Reactivity of Cerebrospinal Fluid-Derived CD4+ T Cells in Multiple Sclerosis

Author

Witold Wolski, Nicole Schaeren-Wiemers, Thomas Zeis, Roland Martin, Mireia Sospedra, Paula Tomas-Ojer, Carla Sellés-Moreno, Marco Puthenparampil, Ivan Jelcic, Bernd Roschitzki, Carolina Cruciani, Wolfgang Faigle, University of Zurich, and Martin, Roland

Subjects

Male, 0301 basic medicine, T-Lymphocytes, multiple sclerosis, T cell reactivity, autoimmune, citrullination, human brain, proteomics, Epitope, chemistry.chemical_compound, Myelin, 0302 clinical medicine, Citrulline, Immunology and Allergy, Original Research, Cerebrospinal Fluid, biology, Chemistry, Brain, Citrullination, Middle Aged, 3. Good health, medicine.anatomical_structure, Proteome, 2723 Immunology and Allergy, Female, Adult, lcsh:Immunologic diseases. Allergy, Adolescent, Immunology, 610 Medicine & health, Young Adult, 03 medical and health sciences, Immune system, medicine, Humans, 2403 Immunology, Multiple sclerosis, Myelin Basic Protein, medicine.disease, 10040 Clinic for Neurology, Myelin basic protein, 030104 developmental biology, biology.protein, Peptides, lcsh:RC581-607, 030215 immunology

Abstract

Immune responses to citrullinated peptides have been described in autoimmune diseases like rheumatoid arthritis (RA) and multiple sclerosis (MS). We investigated the post-translational modification (PTM), arginine to citrulline, in brain tissue of MS patients and controls (C) by proteomics and subsequently the cellular immune response of cerebrospinal fluid (CSF)-infiltrating T cells to citrullinated and unmodified peptides of myelin basic protein (MBP). Using specifically adapted tissue extraction- and combined data interpretation protocols we could establish a map of citrullinated proteins by identifying more than 80 proteins with two or more citrullinated peptides in human brain tissue. We report many of them for the first time. For the already described citrullinated proteins MBP, GFAP, and vimentin, we could identify additional citrullinated sites. The number of modified proteins in MS white matter was higher than control tissue. Citrullinated peptides are considered neoepitopes that may trigger autoreactivity. We used newly identified epitopes and previously reported immunodominant myelin peptides in their citrullinated and non-citrullinated form to address the recognition of CSF-infiltrating CD4+ T cells from 22 MS patients by measuring proliferation and IFN-γ secretion. We did not detect marked responses to citrullinated peptides, but slightly more strongly to the non-modified version. Based on these data, we conclude that citrullination does not appear to be an important activating factor of a T cell response, but could be the consequence of an immune- or inflammatory response. Our approach allowed us to perform a deep proteome analysis and opens new technical possibilities to analyze complex PTM patterns on minute quantities of rare tissue samples. ISSN:1664-3224

Published

2019

13. GDP- <scp>l</scp> -fucose synthase is a CD4 + T cell–specific autoantigen in DRB3*02:02 patients with multiple sclerosis

Author

Mireia Sospedra, Roland Martin, Herena Eixarch, Carolina Cruciani, Raquel Planas, Andreas Lutterotti, Radleigh G. Santos, Clemencia Pinilla, Paula Tomas-Ojer, Wolfgang Faigle, Carmen Espejo, and Nicole Schaeren-Wiemers

Subjects

0301 basic medicine, Autoimmune disease, biology, ATP synthase, Multiple sclerosis, Central nervous system, General Medicine, medicine.disease, Myelin basic protein, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Antigen, chemistry, Guanosine diphosphate, Immunology, biology.protein, medicine, Peptide sequence, 030217 neurology & neurosurgery

Abstract

Multiple sclerosis is an immune-mediated autoimmune disease of the central nervous system that develops in genetically susceptible individuals and likely requires environmental triggers. The autoantigens and molecular mimics triggering the autoimmune response in multiple sclerosis remain incompletely understood. By using a brain-infiltrating CD4 + T cell clone that is clonally expanded in multiple sclerosis brain lesions and a systematic approach for the identification of its target antigens, positional scanning peptide libraries in combination with biometrical analysis, we have identified guanosine diphosphate (GDP)–l-fucose synthase as an autoantigen that is recognized by cerebrospinal fluid–infiltrating CD4 + T cells from HLA-DRB3*–positive patients. Significant associations were found between reactivity to GDP-l-fucose synthase peptides and DRB3*02:02 expression, along with reactivity against an immunodominant myelin basic protein peptide. These results, coupled with the cross-recognition of homologous peptides from gut microbiota, suggest a possible role of this antigen as an inducer or driver of pathogenic autoimmune responses in multiple sclerosis.

Published

2018

14. GDP-l-fucose synthase is a CD4

Author

Raquel, Planas, Radleigh, Santos, Paula, Tomas-Ojer, Carolina, Cruciani, Andreas, Lutterotti, Wolfgang, Faigle, Nicole, Schaeren-Wiemers, Carmen, Espejo, Herena, Eixarch, Clemencia, Pinilla, Roland, Martin, and Mireia, Sospedra

Subjects

CD4-Positive T-Lymphocytes, Multiple Sclerosis, Brain, Myelin Basic Protein, Autoantigens, Clone Cells, Glucosyltransferases, Humans, Amino Acid Sequence, RNA, Messenger, HLA-DRB3 Chains, Peptides, Alleles, Fucose

Abstract

Multiple sclerosis is an immune-mediated autoimmune disease of the central nervous system that develops in genetically susceptible individuals and likely requires environmental triggers. The autoantigens and molecular mimics triggering the autoimmune response in multiple sclerosis remain incompletely understood. By using a brain-infiltrating CD4

Published

2018