Oligodendrocyte precursor cells present antigen and are cytotoxic targets in inflammatory demyelination

Kirby, Leslie; Jin, Jing; Cardona, Jaime Gonzalez; Smith, Matthew D.; Martin, Kenneth E.; Wang, Jingya; Strasburger, Hayley J.; Herbst, Leyla; Alexis, Maya; Karnell, Jodi L.; Davidson, Todd S.; Dutta, Ranjan; Goverman, Joan; Bergles, Dwight E.; Calabresi, Peter A.

doi:10.1038/s41467-019-11638-3

Cited by 262 publications

(297 citation statements)

References 67 publications

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“…Although OPCs are slightly less abundant in the deeper layers compared to the surface 100 μm (Supplementary Figure 3A,C,D) ( p = 2.084 × 10 −13 , N-way ANOVA, by depth), there was no evidence of persistent OPC depletion during recovery (Supplementary Figure 3D,F) ( p = 0.086, Kruskal-Wallis one-way ANOVA). Reactive astrocytes, a known pathological feature of both the cuprizone model and cortical demyelinating lesions (Chang et al, 2012; Skripuletz et al, 2008), can impair OPC differentiation by secreting cytokines (Kirby et al, 2019; Su et al, 2011; Zhang et al, 2010), but whether reactive astrocytes impair recovery differently as a function of cortical depth is unknown. GFAP+ astrocytes are relatively rare in the deeper (200-500 μm) regions of cortex in naïve mice; however, following cuprizone-treatment, their number increased nearly ten-fold ( p = 5.86 × 10 −16 , N-way ANOVA, by time-point).…”

Section: Resultsmentioning

confidence: 99%

“…The inability to recover fully from a demyelinating event raises the possibility that inflammation persists long after the initial trauma, or that OPCs in these regions are permanently altered as a result of exposure to this environment, if only for a short time (Baxi et al, 2015; Kirby et al, 2019). Like other progenitor cells, OPCs exhibit a decline in regenerative potential with age and can undergo senescence, a process that may be accelerated by exposure to inflammatory cytokines (Kirby et al, 2019; Neumann et al, 2019; Nicaise et al, 2019). It is also possible that there is a restricted time period during which OPCs can detect and respond to myelin loss; if there are inherent limits on OPC mobilization, as suggested by the uniform behavior of OPCs across cortical layers, then the inability to match the demand for new cells early may lead to prolonged deficits.…”

Section: Discussionmentioning

confidence: 99%

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Remyelination alters the pattern of myelin in the cerebral cortex

Orthmann-Murphy

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Molina‐Castro

et al. 2020

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37Destruction of oligodendrocytes and myelin sheaths in cortical gray matter profoundly alters 38 neural activity and is associated with cognitive disability in multiple sclerosis (MS). Myelin can 39 be restored by regenerating oligodendrocytes from resident progenitors; however, it is not 40 known whether regeneration restores the complex myelination patterns in cortical circuits. Here 41 we performed time lapse in vivo two photon imaging in somatosensory cortex of adult mice to 42 define the kinetics and specificity of myelin regeneration after acute oligodendrocyte ablation. 43These longitudinal studies revealed that the pattern of myelination in cortex changed 44 dramatically after regeneration, as new oligodendrocytes were formed in different locations and 45 new sheaths were often established along axon segments previously lacking myelin. Despite 46 the dramatic increase in axonal territory available, oligodendrogenesis was persistently impaired 47 in deeper cortical layers that experienced higher gliosis. The repeated reorganization of myelin 48 patterns in MS may alter circuit function and contribute to cognitive decline. 49 50 51 INTRODUCTION 52 53 Oligodendrocytes form concentric sheets of membrane around axons that enhance the speed of 54 action potential propagation, provide metabolic support and control neuronal excitability through 55 ion homeostasis. Consequently, loss of oligodendrocytes and myelin can alter the firing 56 behavior of neurons and impair their survival, leading to profound disability in diseases such as 57 multiple sclerosis (MS), in which the immune system inappropriately targets myelin for 58 destruction. In both relapsing-remitting forms of MS and the cuprizone model of demyelination in 59 mouse, the CNS is capable of spontaneous remyelination through mobilization of 60 oligodendrocyte precursor cells (OPCs) (Baxi et al., 2017; Chang, Nishiyama, Peterson,

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Remyelination alters the pattern of myelin in the cerebral cortex

Orthmann-Murphy

Call

Molina‐Castro

et al. 2020

Preprint

Self Cite

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“…Briefly, striatums were triturated and digested with 1 mg/mL Collagenase IV (Sigma) and 20 μg/mL DNAse I (Sigma) diluted in RPMI 1640 with 10% heat inactivated fetal bovine serum, 1% l-glutamine (Sigma), and 1% Penicillin-Streptomycin (Sigma). Mononuclear cells were separated out using a 30/70% percoll gradient (GE) as previously described [30]. For deep cervical lymph nodes, lymph nodes were isolated and subsequently disassociated through a 70 μm filter.…”

Section: Mononuclear Cell Isolation and Flow Cytometrymentioning

confidence: 99%

T cell infiltration in both human multiple system atrophy and a novel mouse model of the disease

et al. 2020

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Multiple system atrophy (MSA) is a progressive neurodegenerative disorder characterized by abnormal accumulation of alpha-synuclein (α-syn) in oligodendrocytes accompanied by inflammation, demyelination, and subsequent synapse and neuronal loss. Little is known about the mechanisms of neurodegeneration in MSA. However, recent work has highlighted the important role of the immune system to the pathophysiology of other synuclein-related diseases such as Parkinson's disease. In this study, we investigated postmortem brain tissue from MSA patients and control subjects for evidence of immune activation in the brain. We found a significant increase of HLA-DR + microglia in the putamen and substantia nigra of MSA patient tissue compared to controls, as well as significant increases in CD3 + , CD4 + , and CD8 + T cells in these same brain regions. To model MSA in vivo, we utilized a viral vector that selectively overexpresses α-syn in oligodendrocytes (Olig001-SYN) with > 95% tropism in the dorsal striatum of mice, resulting in demyelination and neuroinflammation similar to that observed in human MSA. Oligodendrocyte transduction with this vector resulted in a robust inflammatory response, which included increased MHCII expression on central nervous system (CNS) resident microglia, and infiltration of pro-inflammatory monocytes into the CNS. We also observed robust infiltration of CD4 T cells into the CNS and antigen-experienced CD4 T cells in the draining cervical lymph nodes. Importantly, genetic deletion of TCR-β or CD4 T cells attenuated α-syn-induced inflammation and demyelination in vivo. These results suggest that T cell priming and infiltration into the CNS are key mechanisms of disease pathogenesis in MSA, and therapeutics targeting T cells may be disease modifying.

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“…In pathological conditions, OPCs can upregulate cytokine production in response to IL-17 signaling and greatly contribute to CNS pathogenesis 17 . Surprisingly, OPCs also upregulate antigen presentation machinery in the demyelinating CNS, and can regulate T cell function [18][19][20] . Taken together, these studies illustrate the dynamic role OPCs can play in the adult CNS and build a strong case in support of exploring adult OPCs diversity at the transcriptional level.…”

Section: Adultmentioning

confidence: 99%

Oligomeric amyloid beta prevents myelination in a clusterin-dependent manner

Beiter

Fernández-Castañeda

Rivet-Noor

et al. 2020

Preprint

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Oligodendrocyte progenitor cells (OPCs) are a mitotically active population of glia that comprise approximately 5% of the adult brain. OPCs maintain their proliferative capacity and ability to differentiate in oligodendrocytes throughout adulthood, but relatively few mature oligodendrocytes are produced following developmental myelination. Recent work has begun to demonstrate that OPCs likely perform multiple functions in both homeostasis and disease, and can significantly impact behavioral phenotypes such as food intake and depressive symptoms. However, the exact mechanisms through which OPCs might influence brain function remains unclear. In this work, we demonstrate that OPCs are transcriptionally diverse and separate into three distinct populations in the homeostatic brain. These three groups show distinct transcriptional signatures and enrichment of biological processes unique to individual OPC populations. We have validated these OPC populations using multiple methods, including multiplex RNA in situ hybridization and RNA flow cytometry. This study provides an important resource that profiles the transcriptome of adult OPCs and will provide a significant foundation for further investigation into novel OPC functions.

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Oligodendrocyte precursor cells present antigen and are cytotoxic targets in inflammatory demyelination

Cited by 262 publications

References 67 publications

Remyelination alters the pattern of myelin in the cerebral cortex

Remyelination alters the pattern of myelin in the cerebral cortex

T cell infiltration in both human multiple system atrophy and a novel mouse model of the disease

Oligomeric amyloid beta prevents myelination in a clusterin-dependent manner

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