592 results on '"David A Hafler"'
Search Results
502. Increased IL-12 production in progressive multiple sclerosis: Induction by activated CD4+ T cells via CD40 ligand
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David A. Hafler, Derek R. Smith, Howard L. Weiner, Samia J. Khoury, and Konstantin E. Balashov
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Progressive multiple sclerosis ,CD40 ,Neurology ,biology ,business.industry ,Multiple sclerosis ,medicine ,Cancer research ,Interleukin 12 ,biology.protein ,Neurology (clinical) ,medicine.disease ,business - Published
- 1996
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503. Functional Characterization of Autoreactive T-cells in Acute Disseminated Encephalomyelitis 199
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David A. Hafler, Annette Pohi-Koppe, and Sandra K. Burchett
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business.industry ,Pediatrics, Perinatology and Child Health ,Immunology ,Acute disseminated encephalomyelitis ,Medicine ,business ,medicine.disease ,Virology - Abstract
Functional Characterization of Autoreactive T-cells in Acute Disseminated Encephalomyelitis 199
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- 1996
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504. Multidimensional analysis of the frequencies and rates of cytokine secretion from single cells by quantitative microengravingElectronic supplementary information (ESI) available: Fig. S1–S4 and Table S1. See DOI: 10.1039/b926849a.
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Qing Han, Elizabeth M. Bradshaw, Björn Nilsson, David A. Hafler, and J. Christopher Love
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CYTOKINES ,SECRETION ,QUANTITATIVE research ,BIODIVERSITY ,IMMUNE system ,CHEMICAL processes ,PROTEIN microarrays ,NUMERICAL analysis ,SIMULATION methods & models - Abstract
The large diversity of cells that comprise the human immune system requires methods that can resolve the individual contributions of specific subsets to an immunological response. Microengraving is process that uses a dense, elastomeric array of microwells to generate microarrays of proteins secreted from large numbers of individual live cells (∼104–105cells/assay). In this paper, we describe an approach based on this technology to quantify the rates of secretion from single immune cells. Numerical simulations of the microengraving process indicated an operating regime between 30 min–4 h that permits quantitative analysis of the rates of secretion. Through experimental validation, we demonstrate that microengraving can provide quantitative measurements of both the frequencies and the distribution in rates of secretion for up to four cytokines simultaneously released from individual viable primary immune cells. The experimental limits of detection ranged from 0.5 to 4 molecules/s for IL-6, IL-17, IFNγ, IL-2, and TNFα. These multidimensional measures resolve the number and intensities of responses by cells exposed to stimuli with greater sensitivity than single-parameter assays for cytokine release. We show that cells from different donors exhibit distinct responses based on both the frequency and magnitude of cytokine secretion when stimulated under different activating conditions. Primary T cells with specific profiles of secretion can also be recovered after microengraving for subsequent expansion in vitro. These examples demonstrate the utility of quantitative, multidimensional profiles of single cells for analyzing the diversity and dynamics of immune responses in vitroand for identifying rare cells from clinical samples. [ABSTRACT FROM AUTHOR]
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- 2010
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505. Evaluating the Intrinsic Cysteine Redox-Dependent States of the A-Chain of Human Insulin Using NMR Spectroscopy, Quantum Chemical Calculations, and Mass Spectrometry.
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Alok K. Sharma, Yan Ling, Allison B. Greer, David A. Hafler, Sally C. Kent, Yong Zhang, and Alan C. Rigby
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- 2010
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506. Correlation of Magnetic Resonance Imaging With Immune and Clinical Measures in 45 MS Patients Receiving 20 to 24 MRI Scans Each Over a 1 -Year Period: 1
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David A. Hafler, Howard L. Weiner, Samia J. Khoury, S. S. Ahn, Marika J. Hohol, Liangge Hsu, E. J. Orav, Ferenc A. Jolesz, Ron Kikinis, and C. R.G. Guttman
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Correlation ,Immune system ,medicine.diagnostic_test ,business.industry ,Period (gene) ,Medicine ,Magnetic resonance imaging ,Neurology (clinical) ,Nuclear medicine ,business - Published
- 1995
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507. Modification of immune responses to myelin basic protein (MBP) using altered peptide ligands
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David A. Hafler, Hikoaki Fukaura, Per Höllsberg, Christian Scholz, and Anja Windhagen
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Proteolipid protein 1 ,Immune system ,Neurology ,biology ,Chemistry ,Immunology ,biology.protein ,Immunology and Allergy ,Citrullination ,Neurology (clinical) ,Peptide ligand ,Cell biology ,Myelin basic protein - Published
- 1995
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508. Treatment of multiple sclerosis and other autoimmune diseases by oral tolerance to autoantigens
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Marika J. Hohol, David A. Hafler, Hikoaki Fukaura, Sally C. Kent, Howard L. Weiner, John Orav, and Samia J. Khoury
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Neurology ,business.industry ,Multiple sclerosis ,Immunology ,medicine ,Immunology and Allergy ,Neurology (clinical) ,medicine.disease ,Oral tolerance ,business - Published
- 1995
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509. Switch of autoreactive human T cell clones from a TH2 to a TGFβ1 secreting phenotype with low affinity T-cell receptor stimulating peptide/MHC complex
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David A. Hafler, Hikoaki Fukaura, Anja Windhagen, Christian Scholz, and Alessandro Sette
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Chemistry ,T cell ,Immunology ,T-cell receptor ,Streptamer ,MHC restriction ,Molecular biology ,Phenotype ,medicine.anatomical_structure ,Neurology ,medicine ,Immunology and Allergy ,Cytotoxic T cell ,Neurology (clinical) ,CD8 ,Peptide/MHC Complex - Published
- 1994
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510. In vivo clonal depletion of human myelin basic protein-reactive T cells by T cell vaccination
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Piet Stinissen, Robert Medaer, David A. Hafler, J.W. Zhang, and Jef Raus
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Neurology ,In vivo ,Immunology ,T-cell vaccination ,biology.protein ,Immunology and Allergy ,Neurology (clinical) ,Biology ,Virology ,Myelin basic protein - Published
- 1994
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511. T cell recognition of immunodominant and cryptic proteolipid protein epitopes in humans
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Alessandro Sette, David A. Hafler, Ahmad Al-Sabbagh, Vijay K. Kuchroo, Silva Markovic-Plese, and Hikoaki Fukoara
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medicine.anatomical_structure ,Proteolipid protein 1 ,Neurology ,T cell ,Immunology ,medicine ,Immunology and Allergy ,Neurology (clinical) ,Biology ,Molecular biology ,Epitope - Published
- 1994
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512. Differential activation of cytolysis and proliferation in HTLV-I tax-reactive CD8 T cells by a single amino acid substitution in a T cell receptor contact residue of the peptide antigen
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David A. Hafler, W. Weber, Fernando Dangond, V. Batra, Alessandro Sette, and Per Höllsberg
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Chemistry ,ZAP70 ,Immunology ,T-cell receptor ,CD28 ,Molecular biology ,Cytolysis ,Residue (chemistry) ,Neurology ,Biochemistry ,Immunology and Allergy ,Cytotoxic T cell ,Neurology (clinical) ,IL-2 receptor ,CD8 - Published
- 1994
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513. Cyclophosphamide and MS‐RRR
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Howard L. Weiner, E. J. Orav, David A. Hafler, and David M. Dawson
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Cyclophosphamide ,business.industry ,medicine ,Neurology (clinical) ,Pharmacology ,business ,medicine.drug - Published
- 1994
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514. Intermittent cyclophosphamide pulse therapy in progressive multiple sclerosis: Final report of the Northeast Cooperative Multiple Sclerosis Treatment Group
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James R. Lehrich, A. Turel, G. A. Mackin, R. Butler, B. Sigsbee, Marc Fisher, G. Birnbaum, David A. Hafler, Stephen L. Hauser, E. J. Orav, A. Safran, Y. LaPierre, M. Moore, David M. Dawson, Robert M. Herndon, Howard L. Weiner, and J. McArthur
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Adult ,Male ,medicine.medical_specialty ,Multiple Sclerosis ,Time Factors ,Cyclophosphamide ,medicine.medical_treatment ,Adrenocorticotropic hormone ,Drug Administration Schedule ,law.invention ,Central nervous system disease ,Adrenocorticotropic Hormone ,Randomized controlled trial ,law ,Internal medicine ,medicine ,Humans ,Neurologic Examination ,Chemotherapy ,business.industry ,Multiple sclerosis ,medicine.disease ,Surgery ,Clinical trial ,Regimen ,Treatment Outcome ,Female ,Neurology (clinical) ,business ,Follow-Up Studies ,medicine.drug - Abstract
Previous studies reported that a 2- to 3-week course of IV cyclophosphamide plus adrenocorticotropic hormone (ACTH) induction can temporarily halt progressive MS for a period of 12 months in the majority of patients treated, after which reprogression occurs. The Northeast Cooperative Multiple Sclerosis Treatment Group was formed to determine whether outpatient pulse cyclophosphamide therapy could affect reprogression and whether there were differences between a modified induction regimen and the previously published regimen. Two hundred fifty-six progressive MS patients were randomized into four groups to receive IV cyclophosphamide/ACTH via the previously published versus a modified induction regimen, with or without outpatient IV cyclophosphamide boosters (700 mg/m2 every other month for 2 years). There were blinded evaluations performed every 6 months. Results demonstrate that (1) there were no differences between the modified and the published induction regimens either in terms of initial stabilization or subsequent progression; (2) without boosters, the majority of patients continued to progress; and (3) in patients receiving boosters, there was a statistically significant benefit at 24 months and 30 months (p = 0.04). Time to treatment failure after 1 year was also significantly prolonged in the booster versus the nonbooster group (p = 0.03). Age was the most important variable that correlated with response to therapy in that amelioration of disease progression occurred primarily in patients 40 years of age or younger. Boosters had a significant benefit on time to treatment failure in patients ages 18 to 40, p = 0.003, but not in patients ages 41 to 55, p = 0.97.(ABSTRACT TRUNCATED AT 250 WORDS)
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- 1993
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515. Reply
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David A. Hafler, Kai W. Wucherpfennig, Staley A. Brod, and Howard L. Weiner
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Neurology ,Neurology (clinical) - Published
- 1991
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516. HTLV-1 induced spontaneous T cell clonal proliferation is rapamycin sensitive
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Per Höllsberg, David A. Hafler, Kai W. Wucherpfennig, and Barbara E. Bierer
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medicine.anatomical_structure ,Neurology ,Chemistry ,T cell ,Immunology ,medicine ,Immunology and Allergy ,Neurology (clinical) ,Molecular biology - Published
- 1991
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517. Analysis of αβ and γδ T cell receptors in multiple sclerosis plaques
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Kai W. Wucherpfennig, Jia Newcombe, Christine Keddy, David A. Hafler, Hong Li, and Louise Cuzner
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Neurology ,Multiple sclerosis ,Immunology ,T-cell receptor ,medicine ,Immunology and Allergy ,Neurology (clinical) ,Biology ,medicine.disease - Published
- 1991
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518. Cytokines and Autoimmune Diseases
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Vijay K. Kuchroo, Nora Sarvetnick, David A. Hafler, Lindsay B. Nicholson, Vijay K. Kuchroo, Nora Sarvetnick, David A. Hafler, and Lindsay B. Nicholson
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- Immunology
- Abstract
Leading researchers synthesize scattered experimental data to help develop an intimate understanding of how cytokines and chemokines are involved in the pathogenesis of autoimmune diseases. The many chapters offer critical reviews the basic mechanisms controlling cytokine induction and regulation, as well as the resulting production of proinflammatory and anti-inflammatory cytokines, the former of which induces organ-specific autoimmune diseases. From the vantage of these insights, they address the role of cytokines in a wide variety of autoimmune diseases, uvetis, encephalomyelitis, multiple sclerosis, human type 1 diabetes, rheumatoid arthritis, SLE, and myasthenia gravis. Authoritative and state-of-the-art, Cytokines and Autoimmune Disease highlights the enormous therapeutic potential of cytokine modulation in the treatment of autoimmune disease.
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- 2002
519. Functional gamma chain-associated T cell receptors on cerebrospinal fluid-derived natural killer-like T cell clones
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Jonathan G. Seidman, David A. Hafler, Soon Jin Lee, Deborah Benjamin, Siew-Lan Ang, A D Duby, and G. M. Peterman
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biology ,T cell ,CD3 ,Immunoglobulin gamma-Chains ,Immunology ,T-cell receptor ,Cell ,Receptors, Antigen, T-Cell ,chemical and pharmacologic phenomena ,T lymphocyte ,Articles ,Virology ,Molecular biology ,Clone Cells ,Killer Cells, Natural ,medicine.anatomical_structure ,Immune system ,Antigen ,Cell surface receptor ,medicine ,biology.protein ,Immunology and Allergy ,Humans ,Subacute Sclerosing Panencephalitis ,Cerebrospinal Fluid - Abstract
We have derived 33 independent T cell clones from the cerebrospinal fluid (CSF) of a patient with subacute sclerosing panencephalitis using a single T cell cloning method. 6% (2 of 33) of these clones express the T cell receptor gamma (TCR-gamma) protein and are called CSF TCR-gamma clones. Phenotypic analyses of the CSF TCR-gamma clones indicate that they are WT-31-, CD3+, CD4-, and CD8-. The TCR-gamma protein exists on the cell surface as part of an 85-kD disulphide-linked dimer noncovalently associated with the CD3 polypeptides. The CSF TCR-gamma clones have NK-like activity that can be inhibited by anti-CD3 mAbs. Both CSF TCR-gamma clones proliferated in response to anti-CD3 mAbs coupled to Sepharose beads and/or IL-2. Furthermore, stimulation of one of these clones with anti-CD3 mAbs results in a rapid rise in intracellular calcium. These data suggest that T cells bearing the CD3-TCR-gamma protein complex are functional and play a role in the human immune response.
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- 1987
520. Loss of functional suppression is linked to decreases in circulating suppressor inducer (CD4 + 2H4 +) T Cells in multiple sclerosis
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David A. Hafler, Howard L. Weiner, Chikao Morimoto, and Michel Chofflon
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medicine.medical_specialty ,Multiple Sclerosis ,biology ,Multiple sclerosis ,Pokeweed mitogen ,Immunity ,T lymphocyte ,Immunoglobulin E ,Mixed lymphocyte reaction ,medicine.disease ,T-Lymphocytes, Regulatory ,Molecular biology ,Peripheral blood mononuclear cell ,Endocrinology ,Neurology ,Internal medicine ,biology.protein ,medicine ,Humans ,Biological Assay ,Inducer ,Neurology (clinical) ,Antibody - Abstract
A consistent immunological finding in patients with progressive multiple sclerosis is a loss of functional suppression. We have recently found decreases in suppressor inducer T cells in progressive multiple sclerosis as measured by two-color immunofluorescence using differentiation markers CD4 and 2H4. In the present study, we examined the relationship between functional suppression and circulating CD4+ 2H4+ T cells using a two-stage assay. (1) T cells were stimulated for 7 days with irradiated non-T cells (autologous mixed lymphocyte reaction [AMLR]) and harvested. It has previously been shown that suppressor T cells are generated during the course of the AMLR. (2) The AMLR-generated suppressor T cells were then incubated with mononuclear cells plus pokeweed mitogen, and immunoglobulin (Ig) synthesis was measured. There was less AMLR-induced suppression of IgG synthesis in patients with progressive multiple sclerosis as compared with normal subjects and patients with other neurological diseases. More importantly, there were significant correlations between decreases in circulating CD4+ 2H4+ cells and the AMLR (p = 0.009). Thus, the decreases in functional suppression and the decreases in the AMLR in multiple sclerosis appear tightly linked to CD4+ 2H4+ cells, and their measurement provides a means to monitor suppressor function phenotypically. Decreases in suppressor inducer T cells may in part explain immunoregulatory abnormalities observed in multiple sclerosis.
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- 1988
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521. In Vivo Activated T Lymphocytes in the Peripheral Blood and Cerebrospinal Fluid of Patients with Multiple Sclerosis
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David A. Fox, Stuart F. Schlossman, Ellis L. Reinherz, Mary Elizabeth Manning, David A. Hafler, and Howard L. Weiner
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Adult ,Male ,Pathology ,medicine.medical_specialty ,Multiple Sclerosis ,Adolescent ,T-Lymphocytes ,Lymphocyte Activation ,Cerebrospinal fluid ,Antigen ,In vivo ,Humans ,Medicine ,Aged ,Progressive multiple sclerosis ,business.industry ,Multiple sclerosis ,Antibodies, Monoclonal ,General Medicine ,T lymphocyte ,Middle Aged ,medicine.disease ,Peripheral blood ,Tumor Necrosis Factor Receptor Superfamily, Member 7 ,Antigens, Surface ,Immunology ,Female ,business - Abstract
We found an increase in peripheral-blood lymphocytes bearing the T-cell-specific activation antigen Ta1 in 20 of 35 patients with progressive multiple sclerosis, 4 of 18 patients with stable or improving multiple sclerosis, 1 of 17 patients with other neurologic diseases, and 1 of 14 normal controls (P less than 0.0002, Fisher's exact test). No increases in two other markers of T-cell activation, T113 and the interleukin-2 receptor, were found. In the cerebrospinal fluid, patients with progressive multiple sclerosis (pleocytosis, 3.9 +/- 1.6 cells per cubic millimeter) had 42 +/- 3.0 per cent Ta1+ cells. In contrast, patients with other inflammatory central nervous system diseases (36 +/- 13 cells per cubic millimeter) had 9.6 +/- 1.8 per cent Ta1+ cells (P less than 0.01). In patients with other neurologic diseases without inflammation (0.7 +/- 0.16 cells per cubic millimeter), the percentage of Ta1+ cells was equivalent to that in patients with multiple sclerosis (39 +/- 5.4 per cent), although the absolute number was lower. There was a positive correlation between the presence of Ta1+ cells in the spinal fluid and blood of patients with other neurologic diseases, but not patients with multiple sclerosis. Less than 1 per cent of lymphocytes from the spinal fluid of patients with multiple sclerosis expressed interleukin-2 receptors, as compared with 9.8 per cent of cells from subjects with other inflammatory neurologic diseases (P less than 0.01). These results suggest that the T cells in the spinal fluid of patients with multiple sclerosis may be activated by a different mechanism or in a different temporal sequence from that in patients with other nervous system diseases. Furthermore, the increase in Ta1+ cells in the peripheral blood of patients with multiple sclerosis demonstrates systemic immune activation in the disease; monitoring such cells may provide an objective measure of abnormal immunologic activity.
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- 1985
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522. Investigation of in vivo activated T cells in multiple sclerosis and inflammatory central nervous system diseases
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L. Christenson, Jack L. Strominger, David A. Hafler, Terry B. Strom, Martin E. Hemler, Howard L. Weiner, H M Shapiro, and John M. Williams
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Multiple Sclerosis ,medicine.drug_class ,T-Lymphocytes ,Immunology ,Central nervous system ,Biology ,Lymphocyte Activation ,Monoclonal antibody ,Pathology and Forensic Medicine ,Antigen ,In vivo ,medicine ,Humans ,Immunology and Allergy ,Receptors, Immunologic ,CD40 ,Multiple sclerosis ,Viral encephalitis ,Antibodies, Monoclonal ,Receptors, Interleukin-2 ,DNA ,T lymphocyte ,Flow Cytometry ,medicine.disease ,medicine.anatomical_structure ,Antigens, Surface ,biology.protein ,Encephalitis - Abstract
Monoclonal antibodies have recently been characterized which identify activated T cells at different stages of differentiation. We compared the expression of the late appearing activation antigen defined by monoclonal antibody TS2/7 with the expression of early appearing activation antigens in a group of patients with active multiple sclerosis, encephalitis, non-inflammatory other neurologic diseases, and normal controls. An increase in TS2/7 reactivity of peripheral blood T cells was found in MS patients compared to controls (P less than 0.001), however, there was no increase in the level of early activation antigens. This was in contrast to three patients with viral encephalitis, who had an increase in the early activation antigen 4F2, but minimal, if any, increase in the TS2/7 reactive antigen. This study demonstrates that in vivo, as in vitro, it is possible to identify multiple differentiation stages for activated T cells. Furthermore, the presence of activated T cells in the peripheral blood of multiple sclerosis patients suggests that there is systemic immune activation in MS, and could provide a means to monitor abnormal immunologic activity in MS when these cells are functionally characterized.
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- 1985
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523. Altered blood T-cell subsets in patients with multiple sclerosis
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Robert J. Fallis, David W. Johnson, David A. Hafler, Kenneth A. Ault, Howard L. Weiner, and Stephen L. Hauser
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Central Nervous System ,Pathology ,medicine.medical_specialty ,Multiple Sclerosis ,T-Lymphocytes ,T cell ,Guinea Pigs ,Immunology ,Central nervous system ,Fluorescent Antibody Technique ,Immunoglobulins ,Leukocyte Count ,Mice ,Immune system ,medicine ,Animals ,Humans ,Immunology and Allergy ,Stage (cooking) ,Pleocytosis ,biology ,business.industry ,Multiple sclerosis ,Antibodies, Monoclonal ,medicine.disease ,medicine.anatomical_structure ,Neurology ,biology.protein ,Neurology (clinical) ,Abnormality ,Antibody ,business - Abstract
We have found an alteration in T-cell subsets in patients with active multiple sclerosis, specifically an increase in the T4: T8 ratio. These findings have been reproducibly obtained over the past four years, occurring in the majority of acute patients tested early in the course of an attack and in between 25 and 40% of chronic progressive patients, depending on their stage of illness. These changes correlate with pleocytosis in spinal fluid and with other abnormalities of immune function, such as spontaneous immunoglobulin production. They have been helpful in assessing disease activity in patients being treated on a variety of protocols and as part of research studies of immunoregulatory abnormality in multiple sclerosis, but have not been helpful as a diagnostic test for multiple sclerosis. The decrease of these cells in the peripheral blood of patients with active disease may be secondary to migration of these cells to the central nervous system, where they are sequestered.
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- 1984
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524. The Use of Cyclophosphamide in the Treatment of Multiple Sclerosis
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Howard L. Weiner, Stephen L. Hauser, James R. Lehrich, David A. Hafler, David M. Dawson, and Robert J. Fallis
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Risk ,Oncology ,Clinical Trials as Topic ,medicine.medical_specialty ,Multiple Sclerosis ,Time Factors ,Cyclophosphamide ,business.industry ,General Neuroscience ,Multiple sclerosis ,Adrenocorticotropic hormone ,medicine.disease ,General Biochemistry, Genetics and Molecular Biology ,Placebos ,Adrenocorticotropic Hormone ,History and Philosophy of Science ,Recurrence ,Research Design ,Internal medicine ,medicine ,Humans ,Drug Therapy, Combination ,business ,medicine.drug - Published
- 1984
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525. Immunotherapy of multiple sclerosis
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David A. Hafler and Howard L. Weiner
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Autoimmune disease ,Immunity, Cellular ,Multiple Sclerosis ,business.industry ,medicine.medical_treatment ,Multiple sclerosis ,Lymphocyte ,Immunosuppression ,Disease ,Immunotherapy ,medicine.disease ,Clinical trial ,medicine.anatomical_structure ,Immune system ,Neurology ,Immunology ,medicine ,Humans ,Neurology (clinical) ,business ,Autoantibodies - Abstract
Based on the assumption that multiple sclerosis is an autoimmune disease, a number of clinical trials designed to suppress the immune system or to restore immune balance in multiple sclerosis have been attempted. Depending on the disease category, the clinical goals of immunotherapy differ. Therapeutic goals include improving recovery from acute attacks, preventing or decreasing the number of relapses, and halting the disease in its progressive stage. The ultimate goal of multiple sclerosis therapy is the early treatment of patients in an attempt to halt the onset of progression. Specific strategies of immunotherapy include generation of a suppressor influence, removal of helper/inducer cells, manipulation of activated T cells, manipulation of class II major histocompatibility complex-bearing cells, alteration of lymphocyte traffic, extracorporeal removal of serum factors or cells, and manipulation of antigen-specific cells. Present treatment modalities are beginning to show some efficacy of nonspecific immunosuppression, but these treatments are limited by their toxicities. As the immunotherapy of multiple sclerosis moves to the next stage in the coming years, patients at an earlier stage of their disease will have to be treated, nontoxic forms of therapy developed, clinical trials lengthened, and a laboratory monitor of the disease developed. Given the positive effects of immunotherapy seen thus far in the disease, it is possible that appropriate immunotherapeutic intervention may provide effective treatment for the disease in the future.
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- 1988
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526. Inflammatory cerebrospinal fluid t cells have activation requirements characteristic of cd4+cd45ra- t cells
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Howard L. Weiner, David A. Hafler, Michel Chofflon, and Victor González
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Antigens, Differentiation, T-Lymphocyte ,Interleukin 2 ,medicine.medical_specialty ,T-Lymphocytes ,T cell ,CD3 ,Immunology ,CD2 Antigens ,Biology ,Lymphocyte Activation ,Interleukin 21 ,Immune system ,Antigen ,Internal medicine ,medicine ,Humans ,Immunology and Allergy ,IL-2 receptor ,Receptors, Immunologic ,Cerebrospinal Fluid ,Interleukin 3 ,Inflammation ,Integrin beta1 ,Receptors, Interleukin-2 ,Antigens, Differentiation ,Endocrinology ,medicine.anatomical_structure ,CD4 Antigens ,biology.protein ,Interleukin-2 ,Leukocyte Common Antigens ,Tetradecanoylphorbol Acetate ,medicine.drug - Abstract
It has long been recognized that T cells in the cerebrospinal fluid (CSF) and other inflammatory compartments cannot be stimulated by mitogen and the reason for this has remained unknown. This question was investigated using mononuclear cells (MNC) isolated from the CSF of subjects with multiple sclerosis and other inflammatory brain diseases which predominantly express the CD4 and CDw29 but not CD45RA determinants. CSF and blood cells were stimulated by either the CD3/T cell receptor complex, the CD2 activation pathway, calcium ionophore, or an activator of protein kinase C, phorbol myristate acetate (PMA). CSF MNC proliferated less than blood MNC following stimulation by phytohemagglutinin in subjects with inflammation in the CSF, but not in subjects with non-inflammatory CNS diseases. Moreover, CSF MNC were not induced to proliferate through stimulation of the CD2 pathway by anti-T11(2) + anti-T11(3) monoclonal antibodies (mAb). This was not due to defects in either interleukin 2 receptors, interleukin 2 secretion, or to T cell pre-activation in vivo. Instead, the refractory activation state of inflammatory CSF T cells was corrected by PMA. That CSF contains predominantly CD4+CDw29+CD45RA- cells suggests that PMA may be co-stimulatory with anti-CD2 mAb to activate this population of T cells. This was confirmed in experiments with sorted T cells from normal subjects. These data suggest that the inability of mitogens or anti-CD2 mAb to stimulate inflammatory CSF T cells, which can be corrected by an inducer of protein kinase C, is related to the relative absence of CD4+CD45RA+ cells in the CSF. Alterations of protein kinase C and protein phosphorylation may exist in inflammatory T cell populations that regulate the immune response.
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- 1989
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527. In vivo labeling of blood T cells: Rapid traffic into cerebrospinal fluid in multiple sclerosis
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Howard L. Weiner and David A. Hafler
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Pathology ,medicine.medical_specialty ,Multiple Sclerosis ,Time Factors ,T-Lymphocytes ,Central nervous system ,Cerebrospinal fluid ,Sheep Red Blood Cell Receptor ,In vivo ,Humans ,Medicine ,Cerebrospinal Fluid ,biology ,business.industry ,Multiple sclerosis ,Antibodies, Monoclonal ,Flow Cytometry ,medicine.disease ,Peripheral blood ,Staining ,medicine.anatomical_structure ,Neurology ,Immunology ,biology.protein ,Binding Sites, Antibody ,Neurology (clinical) ,Antibody ,business - Abstract
Multiple sclerosis (MS) is an inflammatory disease of the central nervous system (CNS). In MS patients being treated with anti-T11, a murine monoclonal antibody which recognizes the sheep red blood cell receptor, it was found that peripheral blood T cells were labeled in vivo by the antibody. Furthermore, anti-T11 did not lyse cells or enter the cerebrospinal fluid (CSF). In CSF specimens obtained by serial lumbar punctures from patients with progressive MS who received five daily infusions of anti-T11, 70 +/- 12% of the T cells had mouse antibody bound to their surface by 72 to 96 hours. No in vivo staining of CSF T cells was observed in patients infused with anti-T4, a murine monoclonal antibody that was not found to label T cells in vivo. These results demonstrate that there is rapid movement of lymphocytes from the peripheral blood to the CNS in patients with progressive MS. This rapid trafficking of T cells suggests that the ongoing pathological process within the CNS may be closely linked to the peripheral immune system and may have implications for the monitoring and treatment of MS.
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- 1987
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528. Selective Loss of the Suppressor-Inducer T-Cell Subset in Progressive Multiple Sclerosis
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John F. Daley, David A. Hafler, Howard L. Weiner, Stuart F. Schlossman, Margaret Hagan, Chikao Morimoto, and Norman L. Letvin
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education.field_of_study ,biology ,medicine.drug_class ,business.industry ,Multiple sclerosis ,Lymphocyte ,Suppressor-inducer T cell ,Population ,Cell ,General Medicine ,T lymphocyte ,Monoclonal antibody ,medicine.disease ,medicine.anatomical_structure ,Immunology ,medicine ,biology.protein ,Antibody ,education ,business - Abstract
The T4+ lymphocyte population includes a subset that induces suppressor T lymphocytes (T8+ cells) and can be distinguished by dual-color fluorescence analysis with anti-2H4 and anti-T4 monoclonal antibodies. To investigate the possible role of these cells in multiple sclerosis, we used anti-2H4 antibody to characterize peripheral-blood lymphocyte subsets in 63 patients with multiple sclerosis that was progressive, stable, or acute (relapsing–remitting). Twenty-three of 37 patients with progressive multiple sclerosis had a selective decrease in the number and percentage of peripheral-blood T cells that induce suppressor cells (T4+2H4+ cells), whereas only 3 of 16 patients with stable disease and 2 of 10 patients in the midst of an acute attack had a significant decrease. These selective decreases of circulating T4+2H4+ cells occurred in only 1 of 34 patient controls with other neurologic diseases and in 2 of 50 healthy controls (P
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- 1987
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529. Autoimmunity following viral infection: demonstration of monoclonal antibodies against normal tissue following infection of mice with reovirus and demonstration of shared antigenicity between virus and lymphocytes
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David A. Hafler, Marc Tardieu, M L Powers, Stephen L. Hauser, and Howard L. Weiner
- Subjects
Antigenicity ,medicine.drug_class ,T-Lymphocytes ,viruses ,Lymphocyte ,Immunology ,Nerve Tissue Proteins ,Cross Reactions ,Reoviridae ,Monoclonal antibody ,Epitope ,Virus ,Mice ,Immune system ,Antigen ,Ependyma ,medicine ,Animals ,Immunology and Allergy ,Autoantibodies ,biology ,Antibodies, Monoclonal ,Virology ,Molecular biology ,Clone Cells ,Reoviridae Infections ,Mice, Inbred C57BL ,medicine.anatomical_structure ,Antibody Formation ,biology.protein ,Binding Sites, Antibody ,Antibody - Abstract
Splenic lymphocytes from adult C57BL/6 mice infected with purified reovirus type 1 or 3 particles were fused with NS1 myeloma cells. Approximately 300 clones were obtained from each fusion (type 1 or type 3) and the supernatants from these clones were screened by radioimmunoassay for their ability to bind virus, T lymphocytes, brain, liver, lung tissues and isolated oligodendrocytes and ependymal cells. Approximately 10% of clones (33 and 26 clones, respectively) were positive for each fusion. For reovirus type 1:21% of positive clones bound only virus, 64% bound one of the normal tissues but not virus, and 15% bound both virus and one or more of the normal tissues. For reovirus type 3: 19% of positive clones bound only virus, 73% bound normal tissue only, and 8% bound both virus and normal tissue. Only 3 positive clones were obtained from uninfected control animals. These experiments demonstrate that (a) during the course of an immune response to a virus, autoantibodies are generated which react with a large variety of normal tissues and that (b) there are shared antigenic structures between viral determinants and normal tissue that can be identified by monoclonal antibodies. Although these results suggest two mechanisms by which an autoimmune response may develop following viral infection, the biological significance of these autoreactive monoclonal antibodies remains to be elucidated.
- Published
- 1984
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530. Decreased autologous mixed lymphocyte reaction in multiple sclerosis
- Author
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David A. Hafler, Howard L. Weiner, and Marion Buchsbaum
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Adult ,Male ,Pathology ,medicine.medical_specialty ,Multiple Sclerosis ,Adolescent ,T-Lymphocytes ,Immunology ,Central nervous system ,Text mining ,Antigen ,Active disease ,medicine ,Humans ,Immunology and Allergy ,Autoimmune disease ,business.industry ,Multiple sclerosis ,Middle Aged ,medicine.disease ,Mixed lymphocyte reaction ,Peripheral blood ,medicine.anatomical_structure ,Neurology ,Female ,Neurology (clinical) ,Lymphocyte Culture Test, Mixed ,business - Abstract
The autologous mixed lymphocyte reaction (AMLR) measures the T-cell response to antigens on the surface of autologous non-T-cells. Studies have shown a decreased ability of T-cells to proliferate during the AMLR in a number of autoimmune and viral disorders. The AMLR was studied in 56 patients with multiple sclerosis (MS), a presumed autoimmune disease of the central nervous system, and the response was correlated with T-cell subsets. The AMLR was decreased in active MS patients (3 117 +/- 573 cpm) as compared to inactive patients (5 896 +/- 1 800 cpm) (P less than 0.05) and normal controls (7 782 +/- 1 725 cpm) (P less than 0.01). There was no significant difference between inactive patients and normal controls (P greater than 0.1). A more pronounced difference was also seen when patients with active disease associated with peripheral blood T4/T8 ratios greater than 3.0 (1 045 +/- 223 cpm) were compared with normal controls (P less than 0.01). In addition, MS patients with T4/T8 ratios of less than 1.0 had an increased AMLR (9 256 +/- 1 762 cmp) as compared to patients with either a high T4/T8 ratio (P less than 0.001) or normal ratio (P less than 0.05). Thus, multiple sclerosis patients with clinically active disease have a decreased AMLR which correlates with high T4/T8 ratios in a subgroup of patients.
- Published
- 1985
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531. Sequestration of virus-specific T cells in the cerebrospinal fluid of a patient with varicella zoster viral meningoencephalitis
- Author
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David A. Hafler, Deborah Benjamin, Howard L. Weiner, Jonathan G. Seidman, and Allan D. Duby
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Antigens, Differentiation, T-Lymphocyte ,Male ,Herpesvirus 3, Human ,T-Lymphocytes ,viruses ,T cell ,Immunology ,Clone (cell biology) ,Mumps virus ,Biology ,medicine.disease_cause ,Herpes Zoster ,Herpesviridae ,Virus ,Epitopes ,Immune system ,Meningoencephalitis ,medicine ,Humans ,Immunology and Allergy ,Histocompatibility Antigens Class II ,Varicella zoster virus ,Nucleic Acid Hybridization ,DNA ,Middle Aged ,medicine.disease ,Virology ,Phenotype ,medicine.anatomical_structure ,Neurology ,Neurology (clinical) - Abstract
The frequency of virus-specific T cells in the cerebrospinal fluid of a patient with viral infection of the brain and meninges was determined by using a single-T-cell cloning technique where a representative sampling of T cells was cloned from cerebrospinal fluid of a patient with varicella zoster viral (VZV) meningoencephalitis. That the derived T-cell clone were in fact clonal was shown by demonstrating, on Southern blot analyses, unique rearrangements of the T-cell antigen-receptor β-chain genes of each clone. Five out of the 15 of the T4 + (CD4), 0/4 of the T8 + , and 0/1 of the T4 + T8 + T-cell clones proliferated to VZV, while no clones proliferated to mumps virus or myelin basic protein. There was no clonal expansion of any VZV-reactive T cell in this patient's cerebrospinal fluid. As VZV meningoencephalitis is thought to be due to the reactivation of a dormant herpes zoster viral infection, it can be regarded as a secondary immune response. The presence of different T-cell receptor β-chain gene rearrangements in each T-cell clone suggests that the T-cell response was polyclonal. These results demonstrate that a high frequency of polyclonal, T4 + antigen-specific T cells can be found in a naturaly occurring, localized, immune response.
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- 1989
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532. Phenotypic and functional analysis of T cells cloned directly from the blood and cerebrospinal fluid of patients with multiple sclerosis
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David W. Johnson, Marion Buchsbaum, David A. Hafler, and Howard L. Weiner
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Interleukin 2 ,Multiple Sclerosis ,T-Lymphocytes ,T cell ,Cerebrospinal fluid ,Antigen ,medicine ,Humans ,Cytotoxic T cell ,biology ,Multiple sclerosis ,Brain ,Myelin Basic Protein ,medicine.disease ,Clone Cells ,Myelin basic protein ,Killer Cells, Natural ,Phenotype ,medicine.anatomical_structure ,Neurology ,Immunology ,biology.protein ,Neurology (clinical) ,Clone (B-cell biology) ,Cell Division ,T-Lymphocytes, Cytotoxic ,medicine.drug - Abstract
A single-cell cloning technique was used to analyze both phenotype and function of individual T cells in patients with multiple sclerosis (MS). Blood and cerebrospinal fluid (CSF) lymphocytes were plated at 1 cell per well, stimulated with phytohemagglutinin followed by interleukin 2, and expanded to 3 X 10(6) cells per "clone." More than 90% of the T8 clones generated from patients with MS and controls in both blood and CSF were cytotoxic precursors. There was also a slight decrease in cytotoxic T4 clones in the blood of patients with MS. The cytotoxic precursor frequencies of T cells in the CSF generally reflected those in the blood. In separate experiments, antigen reactivity was examined in lines established from blood or CSF. No reactivity to myelin basic protein or white matter was found in patients with MS or controls. Myelin basic protein-reactive clones could, however, be generated after first stimulating lymphocytes with antigen before cloning. These results suggest that changes in the T8 population from the blood of patients with MS involve cytotoxic as well as suppressor cells. Sequestration of myelin basic protein- or white matter-reactive T cells was not seen in the CSF of patients with MS, unlike reports of viral meningoencephalitis, in which large numbers of antigen-specific cells were found in the CSF. Direct single-cell clonal analysis of the CSF should provide a more sophisticated approach to the study of T cell abnormalities in patients with MS.
- Published
- 1985
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533. Treg Cells Expressing the Coinhibitory Molecule TIGIT Selectively Inhibit Proinflammatory Th1 and Th17 Cell Responses
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Arlene H. Sharpe, David A. Hafler, Chen Zhu, Diane Mathis, Patrick R. Burkett, Christophe Benoist, Francisco J. Quintana, Vijay K. Kuchroo, Nicole Joller, Ester Lozano, Junrong Xia, Bonny Patel, Esen Sefik, Sheng Xiao, Vijay Yajnik, and Tze Guan Tan
- Subjects
Immunology ,Cell ,Mice, Transgenic ,chemical and pharmacologic phenomena ,Biology ,Lymphocyte Activation ,T-Lymphocytes, Regulatory ,Article ,Proinflammatory cytokine ,Mice ,Immune system ,TIGIT ,T-Lymphocyte Subsets ,Respiratory Hypersensitivity ,medicine ,Animals ,Immunology and Allergy ,Receptors, Immunologic ,Th1-Th2 Balance ,Cells, Cultured ,Cell Proliferation ,Immunosuppression Therapy ,Mice, Knockout ,Cell growth ,Effector ,Gene Expression Profiling ,Fibrinogen ,FOXP3 ,Forkhead Transcription Factors ,hemic and immune systems ,Cell biology ,Eosinophils ,Mice, Inbred C57BL ,Infectious Diseases ,medicine.anatomical_structure ,Gene Expression Regulation ,Cytokines - Abstract
SummaryFoxp3+ T regulatory (Treg) cells regulate immune responses and maintain self-tolerance. Recent work shows that Treg cells are comprised of many subpopulations with specialized regulatory functions. Here we identified Foxp3+ T cells expressing the coinhibitory molecule TIGIT as a distinct Treg cell subset that specifically suppresses proinflammatory T helper 1 (Th1) and Th17 cell, but not Th2 cell responses. Transcriptional profiling characterized TIGIT+ Treg cells as an activated Treg cell subset with high expression of Treg signature genes. Ligation of TIGIT on Treg cells induced expression of the effector molecule fibrinogen-like protein 2 (Fgl2), which promoted Treg-cell-mediated suppression of T effector cell proliferation. In addition, Fgl2 was necessary to prevent suppression of Th2 cytokine production in a model of allergic airway inflammation. TIGIT expression therefore identifies a Treg cell subset that demonstrates selectivity for suppression of Th1 and Th17 cell but not Th2 cell responses.
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534. An Autoimmune Disease-Associated CTLA-4 Splice Variant Lacking the B7 Binding Domain Signals Negatively in T Cells
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Arlene H. Sharpe, David A. Hafler, Laurence B. Peterson, Rebecca J. Greenwald, Zsolt Illes, Bernhard Greve, Gordon J. Freeman, Lalitha Vijayakrishnan, Linda S. Wicker, Jacqueline M. Slavik, Vijay K. Kuchroo, and Dan Rainbow
- Subjects
T-Lymphocytes ,T cell ,Blotting, Western ,Molecular Sequence Data ,Immunology ,Receptors, Antigen, T-Cell ,Nod ,Biology ,Autoimmune Diseases ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Antigen ,Antigens, CD ,Mice, Inbred NOD ,medicine ,Animals ,Humans ,Cytotoxic T cell ,Immunology and Allergy ,CTLA-4 Antigen ,Amino Acid Sequence ,RNA, Messenger ,IL-2 receptor ,Cloning, Molecular ,030304 developmental biology ,NOD mice ,Genetics ,0303 health sciences ,Reverse Transcriptase Polymerase Chain Reaction ,Membrane Proteins ,Flow Cytometry ,Antigens, Differentiation ,3. Good health ,Cell biology ,medicine.anatomical_structure ,Infectious Diseases ,CTLA-4 ,B7-1 Antigen ,Female ,Signal Transduction ,030215 immunology ,Binding domain - Abstract
Cytotoxic T lymphocyte-associated antigen-4 (CTLA-4) plays a critical role in downregulating T cell responses. A number of autoimmune diseases have shown genetic linkage to the CTLA-4 locus. We have cloned and expressed an alternatively spliced form of CTLA-4 that has genetic linkage with type I diabetes in the NOD mice. This splice variant of CTLA-4, named ligand-independent CTLA-4 (liCTLA-4), lacks exon2 including the MYPPPY motif essential for binding to the costimulatory ligands B7-1 and B7-2. Here we show that liCTLA-4 is expressed as a protein in primary T cells and strongly inhibits T cell responses by binding and dephosphorylating the TcRζ chain. Expression of liCTLA-4, but not full-length CTLA-4 (flCTLA-4), was higher in memory/regulatory T cells from diabetes-resistant NOD congenic mice compared to susceptible NOD mice. These data suggest that increased expression and negative signaling delivered by the liCTLA-4 may regulate development of T cell-mediated autoimmune diseases.
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535. A High-Density Screen for Linkage in Multiple Sclerosis
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L P Ryder, A. Oturai, L. F. Barcellos, Maria Ban, Andrew Kirby, A Ivinson, Oksenberg, K. M. Myhr, M Laaksonen, Yeo Tw, Pameli Datta, Robin R. Lincoln, Jacqueline Rimmler, David A. Hafler, Stephen L. Hauser, David R. Booth, Stephen Sawcer, Eva Åkesson, Mark J. Daly, Robert Heard, Alastair Compston, Graeme J. Stewart, Eric S. Lander, Simon G. Gregory, Silke Schmidt, Hanne F. Harbo, Anne Spurkland, Shannon J. Kenealy, Emily Walsh, Jonathan L. Haines, Melanie Maranian, John D. Rioux, Margaret A. Pericak-Vance, Jan Hillert, and De Jager Pl
- Subjects
Genetic Markers ,Multiple Sclerosis ,Genetic Linkage ,Locus (genetics) ,Biology ,Genome ,03 medical and health sciences ,symbols.namesake ,0302 clinical medicine ,Genetic linkage ,Genetics ,Chromosomes, Human ,Humans ,Family ,Genetic Predisposition to Disease ,Genetic Testing ,Allele ,Genetics (clinical) ,030304 developmental biology ,0303 health sciences ,Australia ,Chromosome Mapping ,Articles ,Genomics ,Middle Aged ,United States ,Complete linkage ,Human genetics ,Europe ,Mendelian inheritance ,symbols ,Human genome ,030217 neurology & neurosurgery - Abstract
To provide a definitive linkage map for multiple sclerosis, we have genotyped the Illumina BeadArray linkage mapping panel (version 4) in a data set of 730 multiplex families of Northern European descent. After the application of stringent quality thresholds, data from 4,506 markers in 2,692 individuals were included in the analysis. Multipoint nonparametric linkage analysis revealed highly significant linkage in the major histocompatibility complex (MHC) on chromosome 6p21 (maximum LOD score [MLS] 11.66) and suggestive linkage on chromosomes 17q23 (MLS 2.45) and 5q33 (MLS 2.18). This set of markers achieved a mean information extraction of 79.3% across the genome, with a Mendelian inconsistency rate of only 0.002%. Stratification based on carriage of the multiple sclerosis-associated DRB1*1501 allele failed to identify any other region of linkage with genomewide significance. However, ordered-subset analysis suggested that there may be an additional locus on chromosome 19p13 that acts independent of the main MHC locus. These data illustrate the substantial increase in power that can be achieved with use of the latest tools emerging from the Human Genome Project and indicate that future attempts to systematically identify susceptibility genes for multiple sclerosis will have to involve large sample sizes and an association-based methodology.
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536. Meta-analysis identifies common gut microbiota associated with multiple sclerosis
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Qingqi Lin, Yair Dorsett, Ali Mirza, Helen Tremlett, Laura Piccio, Erin E. Longbrake, Siobhan Ni Choileain, David A. Hafler, Laura M. Cox, Howard L. Weiner, Takashi Yamamura, Kun Chen, Yufeng Wu, and Yanjiao Zhou
- Subjects
Meta-analysis ,Microbiota ,Multiple sclerosis ,Prevotella ,Faecalibacterium ,Medicine ,Genetics ,QH426-470 - Abstract
Abstract Background Previous studies have identified a diverse group of microbial taxa that differ between patients with multiple sclerosis (MS) and the healthy population. However, interpreting findings on MS-associated microbiota is challenging, as there is no true consensus. It is unclear whether there is gut microbiota commonly altered in MS across studies. Methods To answer this, we performed a meta-analysis based on the 16S rRNA gene sequencing data from seven geographically and technically diverse studies comprising a total of 524 adult subjects (257 MS and 267 healthy controls). Analysis was conducted for each individual study after reprocessing the data and also by combining all data together. The blocked Wilcoxon rank-sum test and linear mixed-effects regression were used to identify differences in microbial composition and diversity between MS and healthy controls. Network analysis was conducted to identify bacterial correlations. A leave-one-out sensitivity analysis was performed to ensure the robustness of the findings. Results The microbiome community structure was significantly different between studies. Re-analysis of data from individual studies revealed a lower relative abundance of Prevotella in MS across studies, compared to controls. Meta-analysis found that although alpha and beta diversity did not differ between MS and controls, a higher abundance of Actinomyces and a lower abundance of Faecalibacterium were reproducibly associated with MS. Additionally, network analysis revealed that the recognized negative Bacteroides-Prevotella correlation in controls was disrupted in patients with MS. Conclusions Our meta-analysis identified common gut microbiota associated with MS across geographically and technically diverse studies.
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- 2024
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537. Loss of Functional Suppression Is Linked to Decreases in Circulating Suppressor-Inducer (CD4+2H4+) T Cells in Multiple Sclerosis
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David A. Hafler, Howard L. Weiner, and Michel Chofflon
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Antigens, Differentiation, T-Lymphocyte ,CD4-Positive T-Lymphocytes ,Multiple Sclerosis ,Immunology ,T-Lymphocytes, Regulatory ,General Biochemistry, Genetics and Molecular Biology ,law.invention ,History and Philosophy of Science ,law ,Immune Tolerance ,medicine ,Immunology and Allergy ,Humans ,Inducer ,Chemistry ,business.industry ,General Neuroscience ,Multiple sclerosis ,Antibodies, Monoclonal ,T-Lymphocytes, Helper-Inducer ,medicine.disease ,Neurology ,Cancer research ,Suppressor ,Neurology (clinical) ,Lymphocyte Culture Test, Mixed ,business - Published
- 1988
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538. PCR Analysis of DNA from Multiple Sclerosis Patients for the Presence of HTLV-I
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Jennifer H. Richardson, Kai W. Wucherpfenning, N. Endo, Peter Rudge, Angus G. Dalgleish, and David A. Hafler
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Multidisciplinary - Published
- 1989
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539. Neutrophils insert elastase into hepatocytes to regulate calcium signaling in alcohol-associated hepatitis.
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Noriyoshi Ogino, Leite, M. Fatima, Guerra, Mateus T., Emma Kruglov, Hiromitsu Asashima, David A. Hafler, Takeshi Ito, Pereira, João P., Peiffer, Brandon J., Zhaoli Sun, Ehrlich, Barbara E., and Nathanson, Michael H.
- Subjects
- *
LIVER cells , *ELASTASES , *NEUTROPHILS , *CALCIUM channels , *HEPATITIS - Abstract
Neutrophil infiltration occurs in a variety of liver diseases, but it is unclear how neutrophils and hepatocytes interact. Neutrophils generally use granule proteases to digest phagocytosed bacteria and foreign substances or neutralize them in neutrophil extracellular traps. In certain pathological states, granule proteases play a destructive role against the host as well. More recently, nondestructive actions of neutrophil granule proteins have been reported, such as modulation of tissue remodeling and metabolism. Here, we report a completely different mechanism by which neutrophils act nondestructively, by inserting granules directly into hepatocytes. Specifically, elastase-containing granules were transferred to hepatocytes where elastase selectively degraded intracellular calcium channels to reduce cell proliferation without cytotoxicity. In response, hepatocytes increased expression of Serpin E2 and A3, which inhibited elastase activity. Elastase insertion was seen in patient specimens of alcohol-associated hepatitis, and the relationship between elastase-mediated ITPR2 degradation and reduced cell proliferation was confirmed in mouse models. Moreover, neutrophils from patients with alcohol-associated hepatitis were more prone to degranulation and more potent in reducing calcium channel expression than neutrophils from healthy individuals. This nondestructive and reversible action on hepatocytes defines a previously unrecognized role for neutrophils in the transient regulation of epithelial calcium signaling mechanisms. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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540. Refining genetic associations in multiple sclerosis
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Åslaug R. Lorentzen, Bertram Müller-Myhsok, David R. Booth, Jonathan L. Haines, Françoise Clerget-Darpoux, Anne Spurkland, David A. Hafler, P. Villoslada, Bertrand Fontaine, Graeme J. Stewart, An Goris, Stephen Sawcer, Virpi M. Leppä, Tania Mihalova, Daniela Galimberti, Alastair Compston, Xavier Montalban, Margaret A. Pericak-Vance, Hanne F. Harbo, Antje Kroner, Colin M. Graham, A. Oturai, Janna Saarela, Sandra D'Alfonso, A Ivinson, Paola Naldi, Stephen L. Hauser, Tomas Olsson, C M van Duijn, Manuel Comabella, R Q Hintzen, Rita Dobosi, Ingrid Kockum, John D. Rioux, Amie Walton, J. Hoksenberg, P. L. De Jager, L. F. Barcellos, Francesco Cucca, Bénédicte Dubois, Maria Ban, Mark J. Daly, Koen Vandenbroeck, Helle Bach Søndergaard, Laura Bergamaschi, Peter Rieckmann, Neil Robertson, Elisabeth Gulowsen Celius, David Sexton, Robert Heard, Florian Holsboer, Finn Sellebjerg, Marie-Claude Babron, Frank Weber, Leena Peltonen, Stanley Hawkins, Jacob L. McCauley, Isabelle Cournu-Rebeix, J. Hillert, Maria Giovanna Marrosu, Marco Salvetti, A. Palotie, Gillian Ingram, Franca Rosa Guerini, and Clive Hawkins
- Subjects
Empirical data ,medicine.medical_specialty ,Multiple Sclerosis ,Genetic Linkage ,Reflection and Reaction ,Bayesian probability ,Complex disease ,03 medical and health sciences ,0302 clinical medicine ,medicine ,False positive paradox ,Humans ,Genetic Predisposition to Disease ,Psychiatry ,030304 developmental biology ,Genetic association ,0303 health sciences ,business.industry ,Multiple sclerosis ,Chromosome Mapping ,medicine.disease ,3. Good health ,Neurology (clinical) ,business ,True positive rate ,030217 neurology & neurosurgery ,Clinical psychology - Abstract
Genome-wide association studies involve several hundred thousand markers and, even when quality control is scrupulous, are invariably confounded by residual uncorrected errors that can falsely inflate the apparent difference between cases and controls (so-called genomic inflation). As a consequence such studies inevitably generate false positives alongside genuine associations. By use of Bayesian logic and empirical data, the Wellcome Trust Case Control Consortium suggested that association studies in complex disease should involve at least 2000 cases and 2000 controls, at which level they predicted that p values of less than 5×10 −7 would more commonly signify true positives than false positives.
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541. Antibodies to Myelin Basic Protein in Cerebrospinal Fluid of Patients with Multiple Sclerosis
- Author
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K. P. Johnson, Hillel S. Panitch, and David A. Hafler
- Subjects
Pathology ,medicine.medical_specialty ,Oligoclonal band ,biology ,business.industry ,Multiple sclerosis ,medicine.disease ,Myelin basic protein ,Pathogenesis ,Cerebrospinal fluid ,Antigen specific ,Solid phase radioimmunoassay ,Immunology ,medicine ,biology.protein ,Antibody ,business - Abstract
Antibodies of the IgG class directed against myelin basic protein (MBP) were detected by solid phase radioimmunoassay in the cerebrospinal fluid (CSF) of patients with multiple sclerosis (MS). Comparison with controls at equivalent IgG concentrations indicated that the activity detected was due to antibody rather than to nonspecific adherence of IgG. Absorption and blocking studies showed that the reaction was antigen specific for MBP. Antibody was found more frequently in patients with active disease, and less often in patients in remission. There was no correlation with total CSF IgG or the presence of oligoclonal bands on electrophoresis. These findings support the occurrence of an autoimmune response in MS, though its role in pathogenesis of the disease remains obscure.
- Published
- 1980
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542. Secondary immune amplification following live poliovirus immunization in humans
- Author
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Howard L. Weiner, David A. Hafler, David A. Fox, Deborah Benjamin, and M L Blue
- Subjects
Adult ,viruses ,T-Lymphocytes ,Immunology ,Administration, Oral ,Biology ,medicine.disease_cause ,Lymphocyte Activation ,Reoviridae ,Vaccines, Attenuated ,complex mixtures ,Virus ,Pathology and Forensic Medicine ,Immune system ,Antigen ,Immunity ,medicine ,Tetanus Toxoid ,Immunology and Allergy ,Humans ,Antigens, Viral ,Poliovirus ,Toxoid ,Virology ,Vaccination ,Poliovirus Vaccine, Inactivated ,Immunization ,Antigens, Surface - Abstract
Eight subjects inoculated orally with live attenuated poliovirus were investigated to study the effects of live virus infection on human T-cell responses. Proliferation to poliovirus and unrelated recall antigens were measured serially over a 3-week period. Five of eight subjects inoculated demonstrated a clear anamnestic response to poliovirus, but three did not. Only the five subjects demonstrating an anamnestic response to poliovirus were found to have augmented secondary immune responses to two unrelated recall antigens (tetanus toxoid and reovirus) and in the autologous mixed lymphocyte response (AMLR). No consistent changes were found in circulating T-cell surface activation antigens whether or not the subjects responded to poliovirus. These studies suggest that an asymptomatic poliovirus infection associated with immunization in humans can induce nonspecific secondary immune amplification as measured by in vitro T-cell proliferative response. This amplification pathway is a potential mechanism for immune responses against antigens other than those of the infecting virus.
- Published
- 1987
543. Immunohistochemical analysis of suppressor-inducer and helper-inducer T cells in multiple sclerosis brain tissue
- Author
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Howard L. Weiner, David A. Hafler, Chikao Morimoto, Raymond A. Sobel, and Eduardo E. Castro
- Subjects
CD4-Positive T-Lymphocytes ,Multiple Sclerosis ,business.industry ,General Neuroscience ,Multiple sclerosis ,Brain ,Brain tissue ,T-Lymphocytes, Helper-Inducer ,Biology ,medicine.disease ,T-Lymphocytes, Regulatory ,General Biochemistry, Genetics and Molecular Biology ,law.invention ,Immunoenzyme Techniques ,Text mining ,History and Philosophy of Science ,law ,medicine ,Cancer research ,Immunohistochemistry ,Suppressor ,Encephalitis ,Humans ,Inducer ,business - Published
- 1988
544. Anti-CD4 and anti-CD2 monoclonal antibody infusions in subjects with multiple sclerosis. Immunosuppressive effects and human antimouse responses
- Author
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Howard L. Weiner and David A. Hafler
- Subjects
Antigens, Differentiation, T-Lymphocyte ,Immunosuppression Therapy ,Multiple Sclerosis ,business.industry ,General Neuroscience ,Multiple sclerosis ,Anti cd4 ,T-Lymphocytes ,CD2 Antigens ,Antibodies, Monoclonal ,medicine.disease ,General Biochemistry, Genetics and Molecular Biology ,Antibodies, Anti-Idiotypic ,Anti-CD2 Monoclonal Antibody ,History and Philosophy of Science ,Immunology ,Medicine ,Humans ,Receptors, Immunologic ,business - Published
- 1988
545. Immunologic responses of progressive multiple sclerosis patients treated with an anti-T-cell monoclonal antibody, anti-T12
- Author
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Howard L. Weiner, Robert J. Fallis, David A. Hafler, David M. Dawson, Ellis L. Reinherz, and Stuart F. Schlossman
- Subjects
musculoskeletal diseases ,Adult ,Multiple Sclerosis ,medicine.drug_class ,T cell ,medicine.medical_treatment ,T-Lymphocytes ,Immunoglobulins ,Monoclonal antibody ,Prednisone ,medicine ,Humans ,biology ,business.industry ,Multiple sclerosis ,Antibodies, Monoclonal ,Immunotherapy ,T lymphocyte ,Middle Aged ,musculoskeletal system ,medicine.disease ,In vitro ,surgical procedures, operative ,medicine.anatomical_structure ,Immunology ,biology.protein ,Neurology (clinical) ,Antibody ,business ,medicine.drug - Abstract
Twelve patients with progressive MS were treated with a murine IgM pan-T-cell monoclonal antibody reactive against T12, a determinant present on most post-thymic T-cells. Circulating T12 + cells could not be detected from days 1 to 7, although T3 + Til + T12 - cells appeared by day 3. Human anti-mouse antibodies were detected in 78% of patients by day 7 and correlated with a decrease in anti-T12 M Ab blood levels and the reappearance of T12 + cells in the blood. Although there were high levels of anti-T12 MAb in the serum, there were only barely detectable levels in the CSF and no decrease in the proportion of T12+ cells in the CSF with treatment. Immunologic studies demonstrated a decrease of in vitro pokeweed mitogen-driven Ig synthesis on day 3 with an increase on day 10 that consisted in part of human anti-mouse antibodies. Eleven of 12 patients completed therapy. Prednisone was administered with the treatment after mild allergic reactions occurred in the first two patients. Because this was an open phase one study and patients were treated with prednisone, the effect of treatment on the progression of disease is difficult to assess, and no definitive conclusions concerning clinical effects can be made.
- Published
- 1986
546. Oligoclonal T lymphocytes in the cerebrospinal fluid of patients with multiple sclerosis
- Author
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A D Duby, David A. Hafler, Soon Jin Lee, Jonathan G. Seidman, Deborah Benjamin, and Howard L. Weiner
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Multiple Sclerosis ,T cell ,Multiple sclerosis ,T-Lymphocytes ,Immunology ,T-cell receptor ,Receptors, Antigen, T-Cell ,Gene rearrangement ,T lymphocyte ,Articles ,Biology ,medicine.disease ,Herpes Zoster ,Clone Cells ,medicine.anatomical_structure ,Cerebrospinal fluid ,Immune system ,Antigen ,Meningoencephalitis ,medicine ,Immunology and Allergy ,Humans ,Subacute Sclerosing Panencephalitis ,Cerebrospinal Fluid - Abstract
We have investigated the T cell populations in the cerebrospinal fluid (CSF) of chronic progressive multiple sclerosis (MS) patients. Individual T cells from the CSF and blood were cloned before expansion and their clonotypes were defined by analysis of rearranged T cell receptor beta chain and gamma chain genes. 87 T cell clones from blood and CSF of two patients with chronic progressive MS were examined for common TCR gene rearrangement patterns. In one patient, 18 of 28 CSF-derived T cell clones demonstrated common TCR gene rearrangements indicating oligoclonal T cell populations; in the blood, two patterns were found twice among 26 T cell clones. In another patient, 5 of 27 CSF-derived clones had common TCR gene rearrangement patterns. In contrast, no common beta chain rearrangement pattern was found among 67 T cell clones derived from the blood or CSF of a patient with subacute sclerosing panencephalitis, among 20 clones from the CSF of a patient with herpes zoster meningoencephalitis, or among 66 clones from a normal subject. A subject with atypical, fatal MS of 8-mo duration was also studied and did not have oligoclonal T cells in the CSF or blood. These results demonstrate that distinct oligoclonal T cell populations can be found in the CSF immune compartment of subjects with nonmalignant inflammatory disease and they can create a new avenue for the investigation of the specificity of the T cell response within the central nervous system.
- Published
- 1988
547. Immunoregulation in multiple sclerosis
- Author
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Howard L. Weiner, David A. Hafler, and Staley A. Brod
- Subjects
Central Nervous System ,Multiple Sclerosis ,business.industry ,Multiple sclerosis ,T-Lymphocytes ,Immunology ,MEDLINE ,medicine.disease ,Lymphocyte Activation ,Phenotype ,Text mining ,medicine ,Lymphocyte activation ,Humans ,Lymphocyte Culture Test, Mixed ,business - Published
- 1989
548. Activated T-Cells and Antigen Reactivity in the Cerebrospinal Fluid and Blood of Patients with Multiple Sclerosis
- Author
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Howard L. Weiner and David A. Hafler
- Subjects
Cerebrospinal fluid ,Antigen ,business.industry ,Multiple sclerosis ,Immunology ,medicine ,Reactivity (chemistry) ,medicine.disease ,business - Published
- 1987
- Full Text
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549. Distinct molecular forms of human T cell receptor gamma/delta detected on viable T cells by a monoclonal antibody
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David A. Hafler, J. J. van Dongen, E de Vries, R J van de Griend, Peter J. Peters, Jannie Borst, and R. L. H. Bolhuis
- Subjects
Adult ,Antigens, Differentiation, T-Lymphocyte ,Cytotoxicity, Immunologic ,T-Cell Receptor Gamma-Delta ,T cell ,CD3 ,T-Lymphocytes ,Immunology ,Receptors, Antigen, T-Cell ,CD3 Complex ,medicine ,Tumor Cells, Cultured ,Immunology and Allergy ,Cytotoxic T cell ,Humans ,IL-2 receptor ,Antigen-presenting cell ,Child ,biology ,T-cell receptor ,Antibodies, Monoclonal ,Receptors, Antigen, T-Cell, gamma-delta ,Articles ,Molecular biology ,Neoplasm Proteins ,medicine.anatomical_structure ,biology.protein - Abstract
A second type of TCR molecule has been identified on human and murine T lymphocytes, which involves the protein products of the gamma and delta genes. T lymphocytes bearing this receptor may constitute a separate cell lineage with a distinct immune function. We have produced an mAb, which specifically detects human TCR-gamma/delta in native as well as denatured states, this in contrast to previously used anti-gamma chain peptide sera, which only reacted with denatured protein. The receptor occurs in different molecular forms, with or without interchain disulphide bonds, in which a delta chain may or may not be detected by cell surface iodination. The mAb is reactive with all these receptor forms. Therefore, this antibody could be used to determine the expression of TCR-gamma/delta on viable human T lymphocytes. In normal individuals, TCR-gamma/delta was found on a subset composing 2-7% of CD3+ lymphocytes in peripheral blood and 0.1-1.0% in thymus. The majority of these cells do not express the CD4 or CD8 antigens, although a significant percentage of CD8+ cells was found. TCR-gamma/delta+ cells in peripheral blood are resting lymphocytes, as judged by ultrastructural analysis. T cell clones with different receptor types can display MHC-nonrestricted cytolytic activity, which is shown to be induced by the culture conditions, most likely by growth factors such as IL-2. This strongly suggests that TCR-gamma/delta does not play a role in target cell recognition in MHC-nonrestricted cytotoxicity. The anti-TCR-gamma/delta antibody can specifically induce cytotoxic activity in clones expressing the receptor, but in addition inhibit growth factor induced cytotoxicity, which indicates a regulatory role of the TCR-gamma/delta/CD3 complex in MHC-nonrestricted cytotoxicity.
- Published
- 1988
550. Decrease of suppressor inducer (CD4+2H4+) T cells in multiple sclerosis cerebrospinal fluid
- Author
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Howard L. Weiner, Chikao Morimoto, Michel Chofflon, and David A. Hafler
- Subjects
Multiple Sclerosis ,medicine.diagnostic_test ,Multiple sclerosis ,Central nervous system ,T lymphocyte ,T-Lymphocytes, Helper-Inducer ,Biology ,medicine.disease ,Molecular biology ,T-Lymphocytes, Regulatory ,Flow cytometry ,medicine.anatomical_structure ,Cerebrospinal fluid ,Neurology ,Immunology ,medicine ,Cytotoxic T cell ,Humans ,Inducer ,Neurology (clinical) ,CD8 - Abstract
T-lymphocytes in the cerebrospinal fluid of patients with multiple sclerosis are predominantly CD4+ (inducer) as opposed to CD8+ (suppressor/cytotoxic) T cells. The CD4+ lymphocytes can be subdivided into populations that express high densities of the CDw29 (4B4) determinant and have helper inducer function or express high densities of CD45R (2H4) determinant and have suppressor inducer function. In the present study, we characterized the nature of these CD4+ T cells in the cerebrospinal fluid of patients with multiple sclerosis by performing flow cytometric analysis on paired samples of blood and cerebrospinal fluid. There were significantly lower percentages of CD4+2H4+ T cells in the cerebrospinal fluid than in the peripheral blood (p = 0.001, paired t test). In contrast, there were increased percentages of helper inducer (CD4+4B4+) T cells in the cerebrospinal fluid (p = 0.001, paired t test), compared with the peripheral blood. Analysis of subjects with other inflammatory disorders of the central nervous system did not show significant decreases in CD4+2H4+ T cells in cerebrospinal fluid, though in some, decreases were also observed. These results indicate that the CD4+ T cells in the cerebrospinal fluid of patients with multiple sclerosis are predominantly helper inducer, as opposed to suppressor inducer T cells, and that the relative decrease of suppressor inducer cells in the peripheral blood of multiple sclerosis patients is not due to their migration to the cerebrospinal fluid. Furthermore, the increased numbers of helper inducer cells in the cerebrospinal fluid may contribute to local autoimmune processes in the central nervous system compartment of multiple sclerosis patients.
- Published
- 1989
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