Interaction of astrocytes and T cells in physiological and pathological conditions

Xie, Lin; Yang, Shaohua

doi:10.1016/j.brainres.2015.03.026

Cited by 64 publications

(65 citation statements)

References 145 publications

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“…For example, astrocyte-secreted CXCL10 promotes the recruitment and entry of lymphocytes into the CNS, and worsens acute spinal cord demyelination in EAE (56, 57). Indeed, there is a growing appreciation for astrocyte-T cell interactions (58–60). The impact of CNS-resident CD8 T cells on astrocyte functions in aged brains remains to be shown.…”

Section: Discussionmentioning

confidence: 99%

Age-Associated Resident Memory CD8 T Cells in the Central Nervous System Are Primed To Potentiate Inflammation after Ischemic Brain Injury

Ritzel

Crapser

Patel

et al. 2016

The Journal of Immunology

149

122

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Aging is associated with an increase in basal inflammation in the central nervous system (CNS) and an overall decline in cognitive function and poorer recovery following injury. Growing evidence suggests that leukocyte recruitment to the CNS is also increased with normal aging, but to date, no systematic evaluation of these “age-associated” leukocytes have been performed. In this work the effect of aging on CNS leukocyte recruitment was examined. Aging was associated with an increased number of CD45hi leukocytes, primarily composed of conventional CD8+ T cells. These results were strain-independent and seen in both sexes. Intravascular labeling and immunohistology revealed the presence of parenchymal CD8+ T cells in several regions of the brain including the choroid plexus and meninges. These cells had effector memory (CD44+CD62L−) and tissue-resident phenotypes and expressed markers associated with T cell receptor (TCR) activation. Analysis of TCRvβ repertoire usage suggested that entry into the CNS is likely stochastic rather than antigen-driven. Correlational analyses revealed a positive association between CD8 T cell numbers and decreased pro-inflammatory function of microglia. However, the effects of cerebral ischemia and ex-vivo stimulation of these cells dramatically increased production of tumor necrosis factor (TNF), interferon gamma (IFNγ), and monocyte-chemotactic protein-1 (MCP-1/CCL2). Taken together, we identified a novel population of resident memory, immunosurveillant CD8 T cells that represent a hallmark of CNS aging and appear to modify microglia homeostasis under normal conditions, but are primed to potentiate inflammation and leukocyte recruitment following ischemic injury.

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Section: Discussionmentioning

confidence: 99%

Age-Associated Resident Memory CD8 T Cells in the Central Nervous System Are Primed To Potentiate Inflammation after Ischemic Brain Injury

Ritzel

Crapser

Patel

et al. 2016

The Journal of Immunology

149

122

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“…Blood-brain barrier (BBB) leakage contributes significantly to the progression of secondary brain injury after ischemic stroke 1 . Although the primary substrate of BBB injury may involve dysfunction in tight junction proteins within the affected endothelium, emerging data now suggest that gliovascular interactions may also be important.…”

Section: Introductionmentioning

confidence: 99%

Astrocyte-Derived Pentraxin 3 Supports Blood–Brain Barrier Integrity Under Acute Phase of Stroke

Shindo

Maki

Mandeville

et al. 2016

Stroke

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Background and Purpose Pentraxin 3 (PTX3) is released upon inflammatory responses in many organs. However, roles of PTX3 in brain are still mostly unknown. Here we asked whether and how PTX3 contributes to blood-brain barrier (BBB) dysfunction during the acute phase of ischemic stroke. Methods In vivo, spontaneously hypertensive rats were subjected to focal cerebral ischemia by transient middle cerebral artery occlusion. At day 3, brains were analyzed to evaluate the cellular origin of PTX3 expression. Correlations with BBB breakdown were assessed by IgG staining. In vitro, rat primary astrocytes and rat brain endothelial RBE.4 cells were cultured to study the role of astrocyte-derived PTX3 on VEGF-mediated endothelial permeability. Results During the acute phase of stroke, reactive astrocytes in the peri-infarct area expressed PTX3. There was negative correlation between gradients of IgG leakage and PTX3-positive astrocytes. Cell culture experiments showed that astrocyte-conditioned media increased levels of tight junction proteins and reduced endothelial permeability under normal conditions. Removing PTX3 from astrocyte-conditioned media by immunoprecipitation increased endothelial permeability. PTX3 strongly bound VEGF in vitro and was able to decrease VEGF-induced endothelial permeability. Conclusions Astrocytes in peri-infarct areas upregulate PTX3 which may support BBB integrity by regulating VEGF-related mechanisms. This response in astrocytes may comprise a compensatory mechanism for maintaining BBB function after ischemic stroke.

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“…While it is now accepted that PD is a results of an inflammatory episode and subsequent microglia activation, increasing loss of functioning dopaminergic neurons [34], synthesis and release of multiple cytokines, accumulation of toxic substances, subcellular organelle dysfunction and increased effects of invading cells, a loss of BBB integrity, vascular endothelium integrity and astrocyte damage, are strongly implicated in a continuing loss of protective abilities [7,[35][36][37][38][39].…”

Section: Discussionmentioning

confidence: 99%

“…The same can be said for astrocytes, with 'misplacement' of the cells in PD and Alzheimer's disease and their release of deadly molecules [39]. Thus, protective cells can become harmful during inflammatory episodes and, coupled with an influx of immune cells, causes disruption of the BBB which is exacerbated by usually beneficial astrocytes that are mechanistically altered and interact with invading cells [37][38][39][40]. Indeed, our previous research has shown cuffs of T-cells around vessels after endotoxin treatment, as well as ubiquitin and TNFα in vascular endothelial cells, suggesting that perivascular disruption occurs and that cells respond in both self-preservation and destructive manners [5,43].…”

Section: Discussionmentioning

confidence: 99%

Changes in Vascular and Immune Cell Content of an LPS Treated Rat Olfactory Bulb PD Model, Measured by Fluorescence Deconvolution Microscopy

Bick¹,

Poindexter²,

Doursout³

2017

J Cytokine Biol

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Objective: We have previously shown changes in protein, immune cell, nitric oxide a neurotrophic factor content and distribution in the olfactory bulb of an endotoxin-treated rat model, as all these factors have been shown to be involved in neurodegeneration. We expanded our studies by fluorescently imaging smooth muscle actin and endothelial nitric oxide synthase (eNOS), both markers of blood vessels, to investigate loss of vasculature content, as well as imaging locations and quantities of immune cells. The work was performed to shed further light on associations between vessel integrity and immune cell initiated endothelial disruption. Our goal was to demonstrate that cytokine production, NOS induction and immune cell increases, are likely part of the process that leads to a loss of olfaction and dopaminergic signaling and includes vascular perturbations.Methods: Rats were sacrificed following lipopolysaccharide (LPS) treatment. Olfactory bulbs were harvested, sectioned from top to bottom to include the tract and sensory neurons, and probed for markers of inflammation. Inducible nitric oxide synthase (iNOS), neuronal nitric oxide synthase (nNOS), eNOS, interleukin-1 beta (IL-1β), TNF-α, interleukin-6, glial cell derived neurotrophic factor (GDNF) and circulating nitric oxide (NO) were imaged together with tagged macrophages, T-cells, B-cells and neutrophils.Results: Serum NO levels indicated that an inflammatory episode had occurred, being significantly higher in treated animals, with tissue levels of NOS elevated for an extended period of time. Immune cell clusters were seen in a number of areas and the localization of NOS isomers suggests that they have divergent roles in neurodegeneration. For instance, eNOS was associated with blood vessels, iNOS with glial and matrix cells and nNOS with glial cells and neurons. T and B-cell numbers showed a sustained increase; neutrophil numbers rapidly increased then returned to baseline levels; macrophage numbers increased and remained high; LAMP positive cell numbers (NK-cells) increased and remained high; GDNF content increased; IL-6, TNF-α and IL-1β levels all rapidly increased, before dropping to untreated levels, while circulating, NO levels increased dramatically. Of interest, the images of vascular content, immune cell content, eNOS and smooth muscle actin, allowed us to show detrimental interactions between cells, factors and vessels. Our data show that the majority of the vessels were intact, though sections of interest were 'extracted' to reveal possible leaky areas. Specific sites of IL-6 positive lymphocyte clustering were noted around vessels, suggesting that interactions are occurring that lead to disruptions of blood vessel tunicae, allowing the internalization of circulating cells and subsequent cytokine-initiated endothelial cell death. Conclusion:Our findings suggest that protective GDNF and eNOS, which maintains vascular tone, are possibly synthesized too late to combat cytokine initiated neuron damage, glial activation and chronic loss of va...

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Interaction of astrocytes and T cells in physiological and pathological conditions

Cited by 64 publications

References 145 publications

Age-Associated Resident Memory CD8 T Cells in the Central Nervous System Are Primed To Potentiate Inflammation after Ischemic Brain Injury

Age-Associated Resident Memory CD8 T Cells in the Central Nervous System Are Primed To Potentiate Inflammation after Ischemic Brain Injury

Astrocyte-Derived Pentraxin 3 Supports Blood–Brain Barrier Integrity Under Acute Phase of Stroke

Changes in Vascular and Immune Cell Content of an LPS Treated Rat Olfactory Bulb PD Model, Measured by Fluorescence Deconvolution Microscopy

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