ABSTRACT
Microglia are specialized brain macrophages that play numerous roles in tissue homeostasis and response to injury. Colony stimulating factor 1 receptor (CSF1R) is a receptor tyrosine kinase required for the development, maintenance, and proliferation of microglia. Here we show that in adult mice peripheral dosing of function-blocking antibodies to the two known ligands of CSF1R, CSF1, and IL-34, can deplete microglia differentially in white and gray matter regions of the brain, respectively. The regional patterns of depletion correspond to the differential expression of CSF1 and IL-34. In addition, we show that while CSF1 is required to establish microglia in the developing embryo, both CSF1 and IL-34 are required beginning in early postnatal development. These results not only clarify the roles of CSF1 and IL-34 in microglia maintenance, but also suggest that signaling through these two ligands might support distinct sub-populations of microglia, an insight that may impact drug development for neurodegenerative and other diseases.
Subject(s)
Gray Matter/immunology , Interleukins/immunology , Macrophage Colony-Stimulating Factor/immunology , Microglia/immunology , Receptors, Granulocyte-Macrophage Colony-Stimulating Factor/immunology , White Matter/immunology , Animals , Interleukins/genetics , Macrophage Colony-Stimulating Factor/genetics , Mice , Mice, Transgenic , Receptors, Granulocyte-Macrophage Colony-Stimulating Factor/genetics , Signal Transduction/genetics , Signal Transduction/immunologyABSTRACT
Background: Efficient personalized therapy paradigms are needed to modify the disease course and halt gray (GM) and white matter (WM) damage in patients with multiple sclerosis (MS). Presently, promising disease-modifying drugs show impressive efficiency, however, tailored markers of therapy responses are required. Here, we aimed to detect in a real-world setting patients with a more favorable brain network response and immune cell dynamics upon dimethyl fumarate (DMF) treatment. Methods: In a cohort of 78 MS patients we identified two thoroughly matched groups, based on age, disease duration, disability status and lesion volume, receiving DMF (n = 42) and NAT (n = 36) and followed them over 16 months. The rate of cortical atrophy and deep GM volumes were quantified. GM and WM network responses were characterized by brain modularization as a marker of regional and global structural alterations. In the DMF group, lymphocyte subsets were analyzed by flow cytometry and related to clinical and MRI parameters. Results: Sixty percent (25 patients) of the DMF and 36% (13 patients) of the NAT group had disease activity during the study period. The rate of cortical atrophy was higher in the DMF group (-2.4%) compared to NAT (-2.1%, p < 0.05) group. GM and WM network dynamics presented increased modularization in both groups. When dividing the DMF-treated cohort into patients free of disease activity (n = 17, DMFR) and patients with disease activity (n = 25, DMFNR) these groups differed significantly in CD8+ cell depletion counts (DMFR: 197.7 ± 97.1/µl; DMFNR: 298.4 ± 190.6/µl, p = 0.03) and also in cortical atrophy (DMFR: -1.7%; DMFNR: -3.2%, p = 0.01). DMFR presented reduced longitudinal GM and WM modularization and less atrophy as markers of preserved structural global network integrity in comparison to DMFNR and even NAT patients. Conclusions: NAT treatment contributes to a reduced rate of cortical atrophy compared to DMF therapy. However, patients under DMF treatment with a stronger CD8+ T cell depletion present a more favorable response in terms of cortical integrity and GM and WM network responses. Our findings may serve as basis for the development of personalized treatment paradigms.
Subject(s)
CD8-Positive T-Lymphocytes , Cerebral Cortex , Dimethyl Fumarate/administration & dosage , Immunologic Factors/administration & dosage , Multiple Sclerosis , Nerve Net/immunology , Adult , Aged , Aged, 80 and over , CD8-Positive T-Lymphocytes/immunology , CD8-Positive T-Lymphocytes/pathology , Cerebral Cortex/immunology , Cerebral Cortex/pathology , Female , Gray Matter/immunology , Gray Matter/pathology , Humans , Longitudinal Studies , Male , Middle Aged , Multiple Sclerosis/drug therapy , Multiple Sclerosis/immunology , Multiple Sclerosis/pathology , Nerve Net/pathology , White Matter/immunology , White Matter/pathologyABSTRACT
Breakdown of the blood-brain barrier (BBB) and increased immune cell trafficking into the central nervous system (CNS) are hallmarks of the pathogenesis of multiple sclerosis (MS). Platelet endothelial cell adhesion molecule-1 (PECAM-1; CD31) is expressed on cells of the vascular compartment and regulates vascular integrity and immune cell trafficking. Involvement of PECAM-1 in MS pathogenesis has been suggested by the detection of increased levels of soluble PECAM-1 (sPECAM-1) in the serum and CSF of MS patients. Here, we report profound upregulation of cell-bound PECAM-1 in initial (pre-phagocytic) white matter as well as active cortical gray matter MS lesions. Using a human in vitro BBB model we observed that PECAM-1 is not essential for the transmigration of human CD4+ T-cell subsets (Th1, Th1*, Th2, and Th17) across the BBB. Employing an additional in vitro BBB model based on primary mouse brain microvascular endothelial cells (pMBMECs) we show that the lack of endothelial PECAM-1 impairs BBB properties as shown by reduced transendothelial electrical resistance (TEER) and increases permeability for small molecular tracers. Investigating T-cell migration across the BBB under physiological flow by in vitro live cell imaging revealed that absence of PECAM-1 in pMBMECs did not influence arrest, polarization, and crawling of effector/memory CD4+ T cells on the pMBMECs. Absence of endothelial PECAM-1 also did not affect the number of T cells able to cross the pMBMEC monolayer under flow, but surprisingly favored transcellular over paracellular T-cell diapedesis. Taken together, our data demonstrate that PECAM-1 is critically involved in regulating BBB permeability and although not required for T-cell diapedesis itself, its presence or absence influences the cellular route of T-cell diapedesis across the BBB. Upregulated expression of cell-bound PECAM-1 in human MS lesions may thus reflect vascular repair mechanisms aiming to restore BBB integrity and paracellular T-cell migration across the BBB as it occurs during CNS immune surveillance.
Subject(s)
Blood-Brain Barrier/immunology , Endothelium, Vascular/metabolism , Gray Matter/immunology , Multiple Sclerosis/immunology , Platelet Endothelial Cell Adhesion Molecule-1/metabolism , T-Lymphocyte Subsets/immunology , Th1 Cells/immunology , White Matter/immunology , Adult , Animals , Cells, Cultured , Endothelium, Vascular/pathology , Female , Humans , Male , Mice , Mice, Inbred C57BL , Mice, Knockout , Neurogenic Inflammation , Paracrine Communication , Platelet Endothelial Cell Adhesion Molecule-1/genetics , Transendothelial and Transepithelial Migration , Up-RegulationABSTRACT
The grey matter is a central target of pathological processes in neurodegenerative disorders such as Parkinson's and Alzheimer's diseases. The grey matter is often also affected in multiple sclerosis, an autoimmune disease of the central nervous system. The mechanisms that underlie grey matter inflammation and degeneration in multiple sclerosis are not well understood. Here we show that, in Lewis rats, T cells directed against the neuronal protein ß-synuclein specifically invade the grey matter and that this is accompanied by the presentation of multifaceted clinical disease. The expression pattern of ß-synuclein induces the local activation of these T cells and, therefore, determined inflammatory priming of the tissue and targeted recruitment of immune cells. The resulting inflammation led to significant changes in the grey matter, which ranged from gliosis and neuronal destruction to brain atrophy. In humans, ß-synuclein-specific T cells were enriched in patients with chronic-progressive multiple sclerosis. These findings reveal a previously unrecognized role of ß-synuclein in provoking T-cell-mediated pathology of the central nervous system.
Subject(s)
Gray Matter/immunology , Gray Matter/pathology , Multiple Sclerosis, Chronic Progressive/immunology , Multiple Sclerosis, Chronic Progressive/pathology , T-Lymphocytes/immunology , beta-Synuclein/immunology , Animals , Brain/pathology , Cell Movement/immunology , Female , Gene Expression Regulation , Gliosis/pathology , Humans , Inflammation/immunology , Inflammation/pathology , Lymphocyte Activation , Lymphocyte Count , Male , Multiple Sclerosis, Chronic Progressive/blood , Neurodegenerative Diseases/immunology , Neurodegenerative Diseases/pathology , Neurons/pathology , Rats , Rats, Inbred Lew , T-Lymphocytes/metabolism , T-Lymphocytes/pathology , beta-Synuclein/analysis , beta-Synuclein/genetics , beta-Synuclein/metabolismABSTRACT
AIMS: Primary progressive aphasia (PPA) is a clinical syndrome characterized by selective language impairments associated with focal cortical atrophy favouring the language dominant hemisphere. PPA is associated with Alzheimer's disease (AD), frontotemporal lobar degeneration (FTLD) and significant accumulation of activated microglia. Activated microglia can initiate an inflammatory cascade that may contribute to neurodegeneration, but their quantitative distribution in cortical white matter and their relationship with cortical atrophy remain unknown. We investigated white matter activated microglia and their association with grey matter atrophy in 10 PPA cases with either AD or FTLD-TDP pathology. METHODS: Activated microglia were quantified with optical density measures of HLA-DR immunoreactivity in two regions with peak cortical atrophy, and one nonatrophied region within the language dominant hemisphere of each PPA case. Nonatrophied contralateral homologues of the language dominant regions were examined for hemispheric asymmetry. RESULTS: Qualitatively, greater densities of activated microglia were observed in cortical white matter when compared to grey matter. Quantitative analyses revealed significantly greater densities of activated microglia in the white matter of atrophied regions compared to nonatrophied regions in the language dominant hemisphere (P < 0.05). Atrophied regions of the language dominant hemisphere also showed significantly more activated microglia compared to contralateral homologues (P < 0.05). CONCLUSIONS: White matter activated microglia accumulate more in atrophied regions in the language dominant hemisphere of PPA. While microglial activation may constitute a response to neurodegenerative processes in white matter, the resultant inflammatory processes may also exacerbate disease progression and contribute to cortical atrophy.
Subject(s)
Alzheimer Disease , Aphasia, Primary Progressive , Cerebral Cortex , Frontotemporal Dementia , Gray Matter , Microglia/immunology , White Matter , Aged , Alzheimer Disease/immunology , Alzheimer Disease/pathology , Aphasia, Primary Progressive/immunology , Aphasia, Primary Progressive/pathology , Atrophy/immunology , Atrophy/pathology , Cerebral Cortex/immunology , Cerebral Cortex/pathology , Female , Frontotemporal Dementia/immunology , Frontotemporal Dementia/pathology , Gray Matter/immunology , Gray Matter/pathology , Humans , Male , Middle Aged , White Matter/immunology , White Matter/pathologyABSTRACT
AIMS: Experimental data suggest that systemic immune activation may create a pro-inflammatory environment with microglia activation in the central nervous system in the absence of overt inflammation, which in turn may be deleterious in conditions of neurodegenerative disease. The extent to which this is relevant for the human brain is unknown. The central aim of this study is to provide an in-depth characterization of the microglia and macrophage response to systemic inflammation. METHODS: We used recently described markers to characterize the origin and functional states of microglia/macrophages in white and grey matter in patients who died under septic conditions and compared it to those patients without systemic inflammation. RESULTS: We found pro-inflammatory microglia activation in septic patients in the white matter, with very little activation in the grey matter. Using a specific marker for resident microglia (TMEM119), we found that parenchyma microglia were activated and that there was additional recruitment of perivascular macrophages. Pro-inflammatory microglia activation occurred in the presence of homeostatic microglia cells. In contrast to inflammatory or ischaemic diseases of the brain, the anti-inflammatory microglia markers CD163 or CD206 were not expressed in acute sepsis. Furthermore, we found pronounced upregulation of inducible nitric oxide synthase not only in microglia, but also in astrocytes and endothelial cells. CONCLUSION: Our results demonstrate the pronounced effects of systemic inflammation on the human brain and have important implications for the selection of control populations for studies on microglia activation in human brain disease.
Subject(s)
Gray Matter/immunology , Macrophages/immunology , Microglia/immunology , Sepsis/immunology , White Matter/immunology , Adult , Aged , Aged, 80 and over , Female , Gray Matter/pathology , Humans , Male , Middle Aged , Sepsis/pathology , White Matter/pathologyABSTRACT
Previous studies have reported that microglia depletion leads to impairment of synapse formation and these cells rapidly repopulate from CNS progenitors. However, the impact of microglia depletion and repopulation in the long-term state of the CNS environment has not been characterized. Here, we report that acute and synchronous microglia depletion and subsequent repopulation induces gray matter microgliosis, neuronal death in the somatosensory cortex and ataxia-like behavior. We find a type 1 interferon inflammatory signature in degenerating somatosensory cortex from microglia-depleted mice. Transcriptomic and mass cytometry analysis of repopulated microglia demonstrates an interferon regulatory factor 7-driven activation state. Minocycline and anti-IFNAR1 antibody treatment attenuate the CNS type 1 interferon-driven inflammation, restore microglia homeostasis and reduce ataxic behavior. Neither microglia depletion nor repopulation impact neuropathology or T-cell responses during experimental autoimmune encephalomyelitis. Together, we found that acute microglia ablation induces a type 1 interferon activation state of gray matter microglia associated with acute neurodegeneration.
Subject(s)
Cell Death/immunology , Encephalomyelitis, Autoimmune, Experimental/immunology , Gray Matter/immunology , Interferon Type I/immunology , Microglia/immunology , Neurons/immunology , Somatosensory Cortex/immunology , Animals , Anti-Bacterial Agents/pharmacology , Ataxia/immunology , Ataxia/pathology , Encephalomyelitis, Autoimmune, Experimental/pathology , Flow Cytometry , Gene Expression Profiling , Gray Matter/pathology , Homeostasis , Immunohistochemistry , Interferon Regulatory Factor-7/genetics , Interferon Regulatory Factor-7/immunology , Mice , Microscopy, Confocal , Minocycline/pharmacology , Neurons/pathology , Receptor, Interferon alpha-beta/antagonists & inhibitors , Rotarod Performance Test , Somatosensory Cortex/pathologyABSTRACT
BACKGROUND: Anti-myelin oligodendrocyte glycoprotein (MOG) antibody associated disorders frequently manifest as optic neuritis, transverse myelitis, and acute disseminated encephalomyelitis. While their clinical phenotypes overlap with relapsing inflammatory Central nervous system (CNS) conditions such as multiple sclerosis and neuromyelitis optica spectrum disorder, MOG-related syndromes frequently occur in a younger age group. In children, longitudinally extensive transverse myelitis (LETM) is less specific for anti-aquaporin-4 associated neuromyelitis optica spectrum disorder, and has also been reported in pediatric multiple sclerosis, idiopathic transverse myelitis, and acute flaccid myelitis. METHODS: We summarize two patients with positive MOG antibodies and myelitis. RESULTS: We identified two individuals with anti-MOG associated LETM that demonstrate primarily gray matter involvement. Clinically these patients exhibited hyperreflexia and had rapid improvement with immunotherapies. CONCLUSIONS: Anti-MOG diseases can cause LETM with gray matter predominance mimicking acute flaccid myelitis, but clinically these patients can have retained reflexes and respond favorably to immunotherapies.
Subject(s)
Autoantibodies/immunology , Gray Matter/diagnostic imaging , Myelin-Oligodendrocyte Glycoprotein/immunology , Myelitis, Transverse/diagnosis , Myelitis, Transverse/immunology , Adolescent , Diagnosis, Differential , Gray Matter/immunology , Humans , Immunotherapy , Male , Myelitis, Transverse/therapy , Reflex, Abnormal/immunologyABSTRACT
The central nervous system undergoes extensive postnatal synapse remodeling that is critical for the formation of mature neural circuits. In a recent issue of Science, Vainchtein et al. (2018) describe an additional role for astrocyte-derived interleukin-33 (IL-33) in promoting synapse refinement by microglia in the developing brain.
Subject(s)
Gray Matter/metabolism , Interleukin-33/genetics , Interleukin-33/metabolism , Animals , Astrocytes/metabolism , Brain/immunology , Brain/metabolism , Gray Matter/immunology , Humans , Microglia/immunology , Microglia/metabolism , Neurogenesis , Synapses/metabolismABSTRACT
The complement pathway has potential contributions to both white (WM) and grey matter (GM) pathology in Multiple Sclerosis (MS). A quantitative assessment of complement involvement is lacking. Here we describe the use of Tissue MicroArray (TMA) methodology in conjunction with immunohistochemistry to investigate the localization of complement pathway proteins in progressive MS cortical GM and subcortical WM. Antibodies targeting complement proteins C1q, C3b, regulatory proteins C1 inhibitor (C1INH, complement receptor 1 (CR1), clusterin, factor H (FH) and the C5a anaphylatoxin receptor (C5aR) were utilised alongside standard markers of tissue pathology. All stained slides were digitised for quantitative analysis. We found that numbers of cells immunolabelled for HLA-DR, GFAP, C5aR, C1q and C3b were increased in WM lesions (WML) and GM lesions (GML) compared to normal appearing WM (NAWM) and GM (NAGM), respectively. The complement regulators C1INH, CR1, FH and clusterin were more abundant in WM lesions, while the number of C1q+ neurons were increased and the number of C1INH+, clusterin+, FH+ and CR1+ neurons decreased in GM lesions. The number of complement component positive cells (C1q, C3b) correlated with complement regulator expression in WM, but there was no statistical association between complement activation and regulator expression in the GM. We conclude that TMA methodology and quantitative analysis provides evidence of complement dysregulation in MS GML, including an association of the numerical density of C1q+ cells with tissue lesions. Our work confirms that complement activation and dysregulation occur in all cases of progressive MS and suggest that complement may provide potential biomarkers of the disease.
Subject(s)
Brain/immunology , Complement Activation , Multiple Sclerosis/immunology , Tissue Array Analysis/methods , Adult , Aged , Astrocytes/immunology , Astrocytes/pathology , Brain/pathology , Female , Gray Matter/immunology , Gray Matter/pathology , Humans , Immunohistochemistry , Kidney/immunology , Kidney/pathology , Male , Microglia/immunology , Microglia/pathology , Middle Aged , Multiple Sclerosis/pathology , Neurons/immunology , Neurons/pathology , White Matter/immunology , White Matter/pathologyABSTRACT
Approximately half of the human brain is composed of white matter (WM), a specialized tissue housing the axonal projection of neurons and their necessary supporting glial cells. Axons course long distances from their parent soma, have a delicate structure, large surface area and in many cases are dependent upon a uniquely close morphological arrangement with myelinating oligodendrocyte partners; all factors that may predispose them to injury and disease. WM damage is central to a range of well-characterized disorders including multiple sclerosis and spinal cord injury and is also makes a significant contribution to disorders often considered to be largely focused in gray matter; for example, in stroke where ~49% of injury by volume is located in WM. In addition, advances in brain imaging have revealed early, often prodromal, changes in WM structure in most forms of neurodegeneration including Alzheimer's, Huntingdon's and Parkinson's diseases as well as during normal cognitive decline and a variety of behavioral conditions. The significance of the early WM changes for the etiology of these diseases is largely unknown. Subtle, early changes in synaptic function may produce the prodromal WM changes evident in imaging, or WM and gray mater structures may undergo simultaneous reactions to the underlying disease process. However, there are rational mechanisms for the transmission of pathology from WM to gray matter and this article suggests an alternative hypothesis: that WM pathology precedes and to some extent is causal of synaptic dysfunction in many common neurological disorders. Neurological disorders that have their origin or their principle lesion in WM are here defined as "leukopathologies".
Subject(s)
Brain/pathology , Leukocytes/pathology , Nervous System Diseases/pathology , Neuroglia/pathology , White Matter/pathology , Animals , Axons/immunology , Axons/pathology , Brain/immunology , Gray Matter/immunology , Gray Matter/pathology , Humans , Leukocytes/immunology , Nervous System Diseases/immunology , Neuroglia/immunology , White Matter/immunologyABSTRACT
OBJECTIVE: Surgery launches a systemic inflammatory reaction that reaches the brain and associates with immune activation and cognitive decline. Although preclinical studies have in part described this systemic-to-brain signaling pathway, we lack information on how these changes appear in humans. This study examines the short- and long-term impact of abdominal surgery on the human brain immune system by positron emission tomography (PET) in relation to blood immune reactivity, plasma inflammatory biomarkers, and cognitive function. METHODS: Eight males undergoing prostatectomy under general anesthesia were included. Prior to surgery (baseline), at postoperative days 3 to 4, and after 3 months, patients were examined using [11 C]PBR28 brain PET imaging to assess brain immune cell activation. Concurrently, systemic inflammatory biomarkers, ex vivo blood tests on immunoreactivity to lipopolysaccharide (LPS) stimulation, and cognitive function were assessed. RESULTS: Patients showed a global downregulation of gray matter [11 C]PBR28 binding of 26 ± 26% (mean ± standard deviation) at 3 to 4 days postoperatively compared to baseline (p = 0.023), recovering or even increasing after 3 months. LPS-induced release of the proinflammatory marker tumor necrosis factor-α in blood displayed a reduction (41 ± 39%) on the 3rd to 4th postoperative day, corresponding to changes in [11 C]PBR28 distribution volume. Change in Stroop Color-Word Test performance between postoperative days 3 to 4 and 3 months correlated to change in [11 C]PBR28 binding (p = 0.027). INTERPRETATION: This study translates preclinical data on changes in the brain immune system after surgery to humans, and suggests an interplay between the human brain and the inflammatory response of the peripheral innate immune system. These findings may be related to postsurgical impairments of cognitive function. Ann Neurol 2017;81:572-582.
Subject(s)
Brain/immunology , Cognitive Dysfunction/etiology , Gray Matter/immunology , Positron-Emission Tomography/methods , Prostatectomy/adverse effects , Abdomen/surgery , Aged , Biomarkers/metabolism , Brain/diagnostic imaging , Brain/metabolism , Brain/physiopathology , Cognitive Dysfunction/physiopathology , Down-Regulation , Follow-Up Studies , Gray Matter/diagnostic imaging , Gray Matter/metabolism , Gray Matter/physiopathology , Humans , Male , Middle AgedABSTRACT
An interaction between external stressors and intrinsic vulnerability is one of the longest standing pathoaetiological explanations for schizophrenia. However, novel lines of evidence from genetics, preclinical studies, epidemiology and imaging have shed new light on the mechanisms that may underlie this, implicating microglia as a key potential mediator. Microglia are the primary immune cells of the central nervous system. They have a central role in the inflammatory response, and are also involved in synaptic pruning and neuronal remodeling. In addition to immune and traumatic stimuli, microglial activation occurs in response to psychosocial stress. Activation of microglia perinatally may make them vulnerable to subsequent overactivation by stressors experienced in later life. Recent advances in genetics have shown that variations in the complement system are associated with schizophrenia, and this system has been shown to regulate microglial synaptic pruning. This suggests a mechanism via which genetic and environmental influences may act synergistically and lead to pathological microglial activation. Microglial overactivation may lead to excessive synaptic pruning and loss of cortical gray matter. Microglial mediated damage to stress-sensitive regions such as the prefrontal cortex and hippocampus may lead directly to cognitive and negative symptoms, and account for a number of the structural brain changes associated with the disorder. Loss of cortical control may also lead to disinhibition of subcortical dopamine-thereby leading to positive psychotic symptoms. We review the preclinical and in vivo evidence for this model and consider the implications this has for treatment, and future directions.
Subject(s)
Brain/immunology , Inflammation/immunology , Microglia/immunology , Psychological Trauma/immunology , Schizophrenia/immunology , Schizophrenic Psychology , Social Environment , Stress, Psychological/immunology , Animals , Brain/metabolism , Brain/pathology , Brain/physiopathology , Disease Susceptibility , Dopamine/metabolism , Gray Matter/immunology , Gray Matter/metabolism , Gray Matter/pathology , Gray Matter/physiopathology , Hippocampus/immunology , Hippocampus/metabolism , Hippocampus/pathology , Hippocampus/physiopathology , Humans , Neuroglia/immunology , Neuronal Plasticity , Psychological Trauma/metabolism , Psychological Trauma/pathology , Psychological Trauma/physiopathology , Schizophrenia/metabolism , Schizophrenia/pathology , Schizophrenia/physiopathology , Stress, Psychological/metabolism , Stress, Psychological/pathology , Stress, Psychological/physiopathologyABSTRACT
Plasmablasts are a highly differentiated, antibody secreting B cell subset whose prevalence correlates with disease activity in Multiple Sclerosis (MS). For most patients experiencing partial transverse myelitis (PTM), plasmablasts are elevated in the blood at the first clinical presentation of disease (known as a clinically isolated syndrome or CIS). In this study we found that many of these peripheral plasmablasts are autoreactive and recognize primarily gray matter targets in brain tissue. These plasmablasts express antibodies that over-utilize immunoglobulin heavy chain V-region subgroup 4 (VH4) genes, and the highly mutated VH4+ plasmablast antibodies recognize intracellular antigens of neurons and astrocytes. Most of the autoreactive, highly mutated VH4+ plasmablast antibodies recognize only a portion of cortical neurons, indicating that the response may be specific to neuronal subgroups or layers. Furthermore, CIS-PTM patients with this plasmablast response also exhibit modest reactivity toward neuroantigens in the plasma IgG antibody pool. Taken together, these data indicate that expanded VH4+ peripheral plasmablasts in early MS patients recognize brain gray matter antigens. Peripheral plasmablasts may be participating in the autoimmune response associated with MS, and provide an interesting avenue for investigating the expansion of autoreactive B cells at the time of the first documented clinical event.
Subject(s)
Autoantibodies/metabolism , B-Lymphocytes/immunology , Brain/immunology , Multiple Sclerosis/immunology , Plasma Cells/immunology , Adult , Aged , Astrocytes/immunology , Astrocytes/pathology , B-Lymphocytes/pathology , Brain/pathology , Encephalomyelitis, Autoimmune, Experimental/immunology , Encephalomyelitis, Autoimmune, Experimental/pathology , Female , Gray Matter/immunology , Gray Matter/pathology , Humans , Immunoglobulin G/metabolism , Male , Middle Aged , Multiple Sclerosis/pathology , Neuromyelitis Optica/immunology , Neuromyelitis Optica/pathology , Neurons/immunology , Neurons/pathology , Plasma Cells/physiology , Stroke/immunology , Stroke/pathology , Young AdultABSTRACT
Physical activity has been positively associated with gray-matter integrity. In contrast, pro-inflammatory cytokines seem to have negative effects on the aging brain and have been related to dementia. It was investigated whether an inactive lifestyle and high levels of inflammation resulted in smaller gray-matter volumes and predicted cognitive decline across 6 years in a population-based study of older adults (n = 414). Self-reported physical activity (fitness-enhancing, health-enhancing, inadequate) was linked to gray-matter volume, such that individuals with inadequate physical activity had the least gray matter. There were no overall associations between different pro-and anti-inflammatory markers (IL-1ß, IL-6, IL-10, IL-12p40, IL-12p70, G-CSF, and TNF-α) and gray-matter integrity. However, persons with inadequate activity and high levels of the pro-inflammatory marker IL-12p40 had smaller volumes of lateral prefrontal cortex and hippocampus and declined more on the Mini-Mental State Examination test over 6 years compared with physically inactive individuals with low levels of IL-12p40 and to more physically active persons, irrespective of their levels of IL-12p40. These patterns of data suggested that inflammation was particularly detrimental in inactive older adults and may exacerbate the negative effects of physical inactivity on brain and cognition in old age. Hum Brain Mapp 37:3462-3473, 2016. © 2016 Wiley Periodicals, Inc.
Subject(s)
Aging/immunology , Aging/pathology , Cognitive Dysfunction/diagnosis , Cognitive Dysfunction/immunology , Gray Matter/diagnostic imaging , Sedentary Behavior , Aged , Aged, 80 and over , Aging/psychology , Biomarkers/blood , Brain/diagnostic imaging , Brain/immunology , Cognitive Dysfunction/blood , Cohort Studies , Exercise/physiology , Exercise/psychology , Female , Gray Matter/immunology , Humans , Inflammation/diagnostic imaging , Inflammation/physiopathology , Inflammation/psychology , Magnetic Resonance Imaging , Male , Mental Status and Dementia Tests , Middle Aged , Organ Size , Prognosis , Random Allocation , Self ReportABSTRACT
PURPOSE: To longitudinally evaluate the cortical thickness and deep gray matter structures volume, measured from T1 three-dimensional (3D) Gradient echo-weighted imaging, and white matter integrity, assessed from diffusion tensor imaging (DTI) of HIV-positive patients. MATERIALS AND METHODS: Twenty-one HIV-positive patients on stable highly active antiretroviral therapy (HAART) with CD4+ T lymphocytes count >200 cells/mL and viral load <50 copies/mL underwent two magnetic resonance imaging (MRI) scans with a median interval of 26.6 months. None of the patients had HIV-related dementia. T1 3D magnetization prepared rapid gradient echo-weighted imaging and DTI along 30 noncolinear directions were performed using a 1.5 Tesla MR scanner. FreeSurfer was used to perform cortical volumetric reconstruction and segmentation of deep gray matter structures. For tract-based spatial statistics analysis, a white matter skeleton was created, and a permutation-based inference with 5000 permutations, with a threshold of P < 0.05 was used to identify abnormalities in fractional anisotropy (FA). The median, radial, and axial diffusivities were also projected onto the mean FA skeleton. RESULTS: There were no significant differences in cortical thickness, deep gray matter structures volumes or diffusivity parameters between scans at the two time points (considering P < 0.05). CONCLUSION: No longitudinal differences in cortical thickness, deep gray matter volumes, or white matter integrity were observed in an HIV-positive population on stable HAART, with undetectable viral load and high CD4+ T lymphocytes count. J. Magn. Reson. Imaging 2016;44:1262-1269.
Subject(s)
Diffusion Tensor Imaging/methods , Encephalitis, Viral/drug therapy , Encephalitis, Viral/pathology , Gray Matter/pathology , HIV Infections/drug therapy , HIV Infections/pathology , White Matter/pathology , Adult , Antiretroviral Therapy, Highly Active/methods , Encephalitis, Viral/immunology , Female , Gray Matter/immunology , HIV Infections/immunology , Humans , Longitudinal Studies , Male , Middle Aged , Organ Size/immunology , Treatment Outcome , Viral Load/immunology , White Matter/immunologyABSTRACT
Chikungunya, "that which bends up" in the Makonde dialect, is an emerging global health threat, with increasing incidence of neurological complications. Until 2013, Chikungunya infection had been largely restricted to East Africa and the Indian Ocean, with cases within the USA reported to be from foreign travel. However, in 2014, over 1 million suspected cases were reported in the Americas, and a recently infected human could serve as an unwitting reservoir for the virus resulting in an epidemic in the continental USA. Chikungunya infection is increasingly being associated with neurological sequelae. In this study, we sought to understand the role of astrocytes in the neuropathogenesis of Chikungunya infection. Even after virus has been cleared form the circulation, astrocytes were activated with regard to TLR2 expression. In addition, white matter astrocytes were hypertrophic, with increased arbor volume in gray matter astrocytes. Combined, these would alter the number and distribution of synapses that each astrocyte would be capable of forming. These results provide the first evidence that Chikungunya infection induces morphometric and innate immune activation of astrocytes in vivo. Perturbed glia-neuron signaling could be a major driving factor in the development of Chikungunya-associated neuropathology.
Subject(s)
Astrocytes/pathology , Chikungunya Fever/pathology , Gliosis/pathology , Immunity, Innate , Neurons/pathology , Animals , Astrocytes/immunology , Astrocytes/virology , Chikungunya Fever/genetics , Chikungunya Fever/immunology , Chikungunya Fever/virology , Chikungunya virus/immunology , Chikungunya virus/pathogenicity , Disease Models, Animal , Gene Expression , Gliosis/genetics , Gliosis/immunology , Gliosis/virology , Gray Matter/immunology , Gray Matter/pathology , Gray Matter/virology , Host-Pathogen Interactions , Humans , Macaca fascicularis , Neurons/immunology , Neurons/virology , Signal Transduction , Telemetry , Toll-Like Receptor 2/genetics , Toll-Like Receptor 2/immunology , White Matter/immunology , White Matter/pathology , White Matter/virologyABSTRACT
*These authors contributed equally to the work in this manuscript.We have previously identified a distinct class of antibodies expressed by B cells in the cerebrospinal fluid (CSF) of early and established relapsing remitting multiple sclerosis (RRMS) patients that is not observed in healthy donors. These antibodies contain a unique pattern of mutations in six codons along VH4 antibody genes that we termed the antibody gene signature (AGS). In fact, patients who have such B cells in their CSF are identified as either having RRMS or developing RRMS in the future. As mutations in antibody genes increase antibody affinity for particular antigens, the goal for this study was to investigate whether AGS(+) antibodies bind to brain tissue antigens. Single B cells were isolated from the CSF of 10 patients with early or established RRMS. We chose 32 of these B cells that expressed antibodies enriched for the AGS for further study. We generated monoclonal full-length recombinant human antibodies (rhAbs) and used both immunological assays and immunohistochemistry to investigate the capacity of these AGS(+) rhAbs to bind brain tissue antigens. AGS(+) rhAbs did not recognize myelin tracts in the corpus callosum. Instead, AGS(+) rhAbs recognized neuronal nuclei and/or astrocytes, which are prevalent in the cortical gray matter. This pattern was unique to the AGS(+) antibodies from early and established RRMS patients, as AGS(+) antibodies from an early neuromyelitis optica patient did not display the same reactivity. Prevalence of CSF-derived B cells expressing AGS(+) antibodies that bind to these cell types may be an indicator of gray matter-directed autoimmunity in early and established RRMS patients.
Subject(s)
Autoantibodies/immunology , Autoantibodies/metabolism , Autoimmunity/physiology , B-Lymphocytes/immunology , Brain/immunology , Gray Matter/immunology , Multiple Sclerosis, Relapsing-Remitting/immunology , Adult , Animals , Autoantibodies/genetics , Encephalomyelitis, Autoimmune, Experimental/immunology , Female , Glycoproteins/genetics , Glycoproteins/metabolism , HeLa Cells , Humans , Male , Mice , Mice, Transgenic , Middle Aged , Multiple Sclerosis, Relapsing-Remitting/cerebrospinal fluid , Oligodendroglia/immunology , Oligodendroglia/metabolism , Recombinant Proteins/metabolism , Stroke/immunology , Young AdultABSTRACT
Multiple sclerosis (MS) is a debilitating disease characterized by demyelination of the central nervous system (CNS), resulting in widespread formation of white matter lesions (WMLs) and grey matter lesions (GMLs). WMLs are pathologically characterized by the presence of immune cells that infiltrate the CNS, whereas these immune cells are barely present in GMLs. This striking pathological difference between WMLs and GMLs raises questions about the underlying mechanism. It is known that infiltrating leukocytes contribute to the generation of WMLs; however, since GMLs show a paucity of infiltrating immune cells, their importance in GML formation remains to be determined. Here, we review pathological characteristics of WMLs and GMLs, and suggest some possible explanations for the observed pathological differences. In our view, cellular and molecular characteristics of WM and GM, and local differences within WMLs and GMLs (in particular, in glial cell populations and the molecules they express), determine the pathway to demyelination. Further understanding of GML pathogenesis, considered to contribute to chronic MS, may have a direct impact on the development of novel therapeutic targets to counteract this progressive neurological disorder.
