Exercise alters LPS-induced glial activation in the mouse brain

Bibiana C. Mota; Áine M. Kelly

doi:10.1042/ns20200003

Exercise alters LPS-induced glial activation in the mouse brain

Neuronal Signaling ◽

10.1042/ns20200003 ◽

2020 ◽

Vol 4 (4) ◽

Author(s):

Bibiana C. Mota ◽

Áine M. Kelly

Keyword(s):

Treadmill Running ◽

Alternative Activation ◽

Spatial Learning And Memory ◽

Cellular Mechanisms ◽

Proinflammatory Response ◽

Systemic Injection ◽

Prior Exercise ◽

Microglial Response ◽

The Brain ◽

Modifiable Lifestyle Factors

Abstract Experimental and epidemiological evidence suggest that modifiable lifestyle factors, including physical exercise, can build structural and cognitive reserve in the brain, increasing resilience to injury and insult. Accordingly, exercise can reduce the increased expression of proinflammatory cytokines in the brain associated with ageing or experimentally induced neuroinflammation. However, the cellular mechanisms by which exercise exerts this effect are unknown, including the effects of exercise on classic or alternative activation of astrocytes and microglia. In the present study, we assess the effects of nine consecutive days of treadmill running on the glial cell response to a single systemic injection of lipopolysaccharide (LPS) and, in parallel, the effects on spatial learning and memory. We show that prior exercise protects against LPS-induced impairment of performance in the object displacement task concomitant with attenuation of IL-1β, TNFα and IL-10 mRNA expression in the hippocampus. Assessment of isolated astrocytes and microglia revealed that LPS induced a proinflammatory response in these cells that was not observed in cells prepared from the brains of mice who had undergone prior exercise. The results suggest that exercise modulates neuroinflammation by reducing the proinflammatory microglial response, suggesting a mechanism by which exercise may be neuroprotective.

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A Destruction Model of the Vascular and Lymphatic Systems in the Emergence of Psychiatric Symptoms

Biology ◽

10.3390/biology10010034 ◽

2021 ◽

Vol 10 (1) ◽

pp. 34

Author(s):

Kohei Segawa ◽

Yukari Blumenthal ◽

Yuki Yamawaki ◽

Gen Ohtsuki

Keyword(s):

Neurodegenerative Diseases ◽

Lymphatic System ◽

Psychiatric Symptoms ◽

Neurological Diseases ◽

Immune Surveillance ◽

Brain Network ◽

Cellular Mechanisms ◽

Postmortem Brains ◽

New Interpretation ◽

The Brain

The lymphatic system is important for antigen presentation and immune surveillance. The lymphatic system in the brain was originally introduced by Giovanni Mascagni in 1787, while the rediscovery of it by Jonathan Kipnis and Kari Kustaa Alitalo now opens the door for a new interpretation of neurological diseases and therapeutic applications. The glymphatic system for the exchanges of cerebrospinal fluid (CSF) and interstitial fluid (ISF) is associated with the blood-brain barrier (BBB), which is involved in the maintenance of immune privilege and homeostasis in the brain. Recent notions from studies of postmortem brains and clinical studies of neurodegenerative diseases, infection, and cerebral hemorrhage, implied that the breakdown of those barrier systems and infiltration of activated immune cells disrupt the function of both neurons and glia in the parenchyma (e.g., modulation of neurophysiological properties and maturation of myelination), which causes the abnormality in the functional connectivity of the entire brain network. Due to the vulnerability, such dysfunction may occur in developing brains as well as in senile or neurodegenerative diseases and may raise the risk of emergence of psychosis symptoms. Here, we introduce this hypothesis with a series of studies and cellular mechanisms.

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Arginase in Parasitic Infections: Macrophage Activation, Immunosuppression, and Intracellular Signals

Journal of Biomedicine and Biotechnology ◽

10.1155/2010/683485 ◽

2010 ◽

Vol 2010 ◽

pp. 1-10 ◽

Cited By ~ 47

Author(s):

Cinthia C. Stempin ◽

Laura R. Dulgerian ◽

Vanina V. Garrido ◽

Fabio M. Cerban

Keyword(s):

Macrophage Activation ◽

Transforming Growth Factor ◽

Parasite Clearance ◽

Alternative Activation ◽

Parasitic Infections ◽

Activated Macrophages ◽

Proinflammatory Response ◽

Alternatively Activated Macrophages ◽

Arginase 1

A type 1 cytokine-dependent proinflammatory response inducing classically activated macrophages (CaMϕs) is crucial for parasite control during protozoan infections but can also contribute to the development of immunopathological disease symptoms. Type 2 cytokines such as IL-4 and IL-13 antagonize CaMϕs inducing alternatively activated macrophages (AaMϕs) that upregulate arginase-1 expression. During several infections, induction of arginase-1-macrophages was showed to have a detrimental role by limiting CaMϕ-dependent parasite clearance and promoting parasite proliferation. Additionally, the role of arginase-1 in T cell suppression has been explored recently. Arginase-1 can also be induced by IL-10 and transforming growth factor-β(TGF-β) or even directly by parasites or parasite components. Therefore, generation of alternative activation states of macrophages could limit collateral tissue damage because of excessive type 1 inflammation. However, they affect disease outcome by promoting parasite survival and proliferation. Thus, modulation of macrophage activation may be instrumental in allowing parasite persistence and long-term host survival.

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In progressive nephropathies, overload of tubular cells with filtered proteins translates glomerular permeability dysfunction into cellular signals of interstitial inflammation.

Journal of the American Society of Nephrology ◽

10.1681/asn.v971213 ◽

1998 ◽

Vol 9 (7) ◽

pp. 1213-1224 ◽

Cited By ~ 2

Author(s):

M Abbate ◽

C Zoja ◽

D Corna ◽

M Capitanio ◽

T Bertani ◽

...

Keyword(s):

Time Course ◽

Early Stage ◽

Protein Accumulation ◽

Glomerular Injury ◽

Cellular Mechanisms ◽

Proinflammatory Response ◽

Glomerular Permeability ◽

Tubular Cells ◽

Interstitial Inflammation ◽

Tubulointerstitial Lesions

Progression to end-stage renal failure is the final common pathway of many forms of glomerular disease, independent of the type of initial insult. Progressive glomerulopathies have in common persistently high levels of urinary protein excretion and tubulointerstitial lesions at biopsy. Among the cellular mechanisms that may determine progression regardless of etiology, the traffic of excess proteins filtered from glomerulus in renal tubule may have functional importance by initiating interstitial inflammation in the early phase of parenchymal injury. This study analyzes the time course and sites of protein accumulation and interstitial cellular infiltration in two different models of proteinuric nephropathies. In remnant kidneys after 5/6 renal mass ablation, albumin and IgG accumulation by proximal tubular cells was visualized in the early stage, preceding interstitial infiltration of MHC-II-positive cells and macrophages. By double-staining, infiltrates developed at or near tubules containing intracellular IgG or luminal casts. This relationship persisted thereafter despite more irregular distribution of infiltrate. Similar patterns were found in an immune model (passive Heymann nephritis), indicating that the interstitial inflammatory reaction develops at the sites of protein overload, regardless of the type of glomerular injury. Osteopontin was detectable in cells of proximal tubules congested with protein in both models at sites of interstitial infiltration, and by virtue of its chemoattractive action this is likely mediator of a proximal tubule-dependent inflammatory pathway in response to protein load. Protein overload of tubules is a key candidate process translating glomerular protein leakage into cellular signals of interstitial inflammation. Mechanisms underlying the proinflammatory response of tubular cells to protein challenge in diseased kidney should be explored, as well as ways of limiting protein reabsorption/deposition to prevent consequent inflammation and progressive disease.

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Reappearance of Hippocampal CA1 Neurons after Ischemia is Associated with Recovery of Learning and Memory

Journal of Cerebral Blood Flow & Metabolism ◽

10.1038/sj.jcbfm.9600153 ◽

2005 ◽

Vol 25 (12) ◽

pp. 1586-1595 ◽

Cited By ~ 117

Author(s):

Olof Bendel ◽

Tjerk Bueters ◽

Mia von Euler ◽

Sven Ove Ögren ◽

Johan Sandin ◽

...

Keyword(s):

Cerebral Ischemia ◽

Learning And Memory ◽

Spatial Learning ◽

Cognitive Functions ◽

Spatial Learning And Memory ◽

Neuronal Marker ◽

Ca1 Neurons ◽

Ca1 Region ◽

Hippocampal Ca1 ◽

The Brain

The pyramidal neurons of the hippocampal CA1 region are essential for cognitive functions such as spatial learning and memory, and are selectively destroyed after cerebral ischemia. To analyze whether degenerated CA1 neurons are replaced by new neurons and whether such regeneration is associated with amelioration in learning and memory deficits, we have used a rat global ischemia model that provides an almost complete disappearance (to approximately 3% of control) of CA1 neurons associated with a robust impairment in spatial learning and memory at two weeks after ischemia. We found that transient cerebral ischemia can evoke a massive formation of new neurons in the CA1 region, reaching approximately 40% of the original number of neurons at 90 days after ischemia (DAI). Co-localization of the mature neuronal marker neuronal nuclei with 5-bromo-2'-deoxyuridine in CA1 confirmed that neurogenesis indeed had occurred after the ischemic insult. Furthermore, we found increased numbers of cells expressing the immature neuron marker polysialic acid neuronal cell adhesion molecule in the adjacent lateral periventricular region, suggesting that the newly formed neurons derive from this region. The reappearance of CA1 neurons was associated with a recovery of ischemia-induced impairments in spatial learning and memory at 90 DAI, suggesting that the newly formed CA1 neurons restore hippocampal CA1 function. In conclusion, these results show that the brain has an endogenous capacity to form new nerve cells after injury, which correlates with a restoration of cognitive functions of the brain.

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Entry of antiepileptic drugs (valproate and lamotrigine) into the developing rat brain

F1000Research ◽

10.12688/f1000research.52607.1 ◽

2021 ◽

Vol 10 ◽

pp. 384

Author(s):

Samuel J. Toll ◽

Fiona Qiu ◽

Yifan Huang ◽

Mark D. Habgood ◽

Katarzyna M. Dziegielewska ◽

...

Keyword(s):

Antiepileptic Drug ◽

Placental Transfer ◽

Rat Plasma ◽

Developing Brain ◽

Adult Brain ◽

Cellular Mechanisms ◽

Antiepileptic Drug Treatment ◽

Dose Dependent ◽

The Brain ◽

Drug Entry

Background: Women with epilepsy face difficult choices whether to continue antiepileptic drug treatment during pregnancy, as uncontrolled seizures carry great risk to mother and fetus but continuing treatment may have adverse effects on baby’s development. This study aimed at evaluating antiepileptic drug entry into developing brain. Methods: Anaesthetised pregnant, non-pregnant adult females, postnatal and fetal rats were injected intraperitoneally with different doses, single or in combinations, of valproate and lamotrigine, all within clinical range. Injectate included 3H-labelled drug. After 30min, CSF, blood and brain samples were obtained; radioactivity was measured using liquid scintillation counting. Some animals were also exposed to valproate in feed throughout pregnancy and into neonatal period. Drug levels were measured by liquid chromatography coupled to mass spectrometry (LC-MS). Results are given as CSF or tissue/plasma% as index of drug entry. Results: Entry of valproate into brain and CSF was higher at E19 and P4 compared to adult but was not dose-dependent; placental transfer increased significantly at highest dose of 100mg/Kg. Lamotrigine entry into the brain was dose dependent only at E19. Chronic valproate treatment, or combination of valproate and lamotrigine had little effect on either drug entry, except for reduced valproate brain entry in adult brain with chronic treatment. Placental transfer decreased significantly after chronic valproate treatment. LC-MS measurement of valproate in adults confirmed that rat plasma values were within the clinical range and CSF/plasma and brain/plasma ratios for LC-MS and 3H-valproate were similar. Conclusion: Results suggest that entry of valproate may be higher in developing brain, the capacity of barrier mechanism is mostly unaffected by doses within the clinical range, with or without addition of lamotrigine. Chronic valproate exposure may result in upregulation in cellular mechanisms restricting its entry into the brain. Entry of lamotrigine was little different at different ages and was not dose dependent.

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Age-Dependent Changes in the Plasma and Brain Pharmacokinetics of Amyloid-β Peptides and Insulin

Journal of Alzheimer s Disease ◽

10.3233/jad-215128 ◽

2021 ◽

pp. 1-14

Author(s):

Andrew L. Zhou ◽

Nidhi Sharda ◽

Vidur V. Sarma ◽

Kristen M. Ahlschwede ◽

Geoffry L. Curran ◽

...

Keyword(s):

Neurodegenerative Disorder ◽

Single Photon ◽

Photon Emission ◽

Amyloid Β ◽

Emission Computed Tomography ◽

Systemic Injection ◽

Age Related ◽

Age Dependent ◽

Plasma Pharmacokinetics ◽

The Brain

Background: Age is the most common risk factor for Alzheimer’s disease (AD), a neurodegenerative disorder characterized by the hallmarks of toxic amyloid-β (Aβ) plaques and hyperphosphorylated tau tangles. Moreover, sub-physiological brain insulin levels have emerged as a pathological manifestation of AD. Objective: Identify age-related changes in the plasma disposition and blood-brain barrier (BBB) trafficking of Aβ peptides and insulin in mice. Methods: Upon systemic injection of 125I-Aβ 40, 125I-Aβ 42, or 125I-insulin, the plasma pharmacokinetics and brain influx were assessed in wild-type (WT) or AD transgenic (APP/PS1) mice at various ages. Additionally, publicly available single-cell RNA-Seq data [GSE129788] was employed to investigate pathways regulating BBB transport in WT mice at different ages. Results: The brain influx of 125I-Aβ 40, estimated as the permeability-surface area product, decreased with age, accompanied by an increase in plasma AUC. In contrast, the brain influx of 125I-Aβ 42 increased with age, accompanied by a decrease in plasma AUC. The age-dependent changes observed in WT mice were accelerated in APP/PS1 mice. As seen with 125I-Aβ 40, the brain influx of 125I-insulin decreased with age in WT mice, accompanied by an increase in plasma AUC. This finding was further supported by dynamic single-photon emission computed tomography (SPECT/CT) imaging studies. RAGE and PI3K/AKT signaling pathways at the BBB, which are implicated in Aβ and insulin transcytosis, respectively, were upregulated with age in WT mice, indicating BBB insulin resistance. Conclusion: Aging differentially affects the plasma pharmacokinetics and brain influx of Aβ isoforms and insulin in a manner that could potentially augment AD risk.

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Altered Calcium Homeostasis During Aging of the Brain: Cellular Mechanisms Involved and Possible Consequences

Neuroregulatory Mechanisms in Aging ◽

10.1016/b978-0-08-041989-3.50009-3 ◽

1993 ◽

pp. 79-88 ◽

Cited By ~ 2

Author(s):

JORGINA SATRÚSTEGUI ◽

ALBERTO MARTÍNEZ-SERRANO ◽

PABLO BLANCO ◽

MARTÍN VILLALBA ◽

PAULINO GÓMEZ PUERTAS ◽

...

Keyword(s):

Calcium Homeostasis ◽

Cellular Mechanisms ◽

The Brain

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Cortical Mechanisms for Emotional Fear and Chronic Pain

European Psychiatry ◽

10.1016/s0924-9338(09)70318-9 ◽

2009 ◽

Vol 24 (S1) ◽

pp. 1-1

Author(s):

M. Zhuo

Keyword(s):

Chronic Pain ◽

Emotional Disorders ◽

Cortical Neurons ◽

Neural Mechanism ◽

Anterior Cingulate ◽

Cellular Mechanisms ◽

New Genes ◽

Trace Fear ◽

The Brain ◽

Synaptic Model

Investigation of molecular and cellular mechanisms of synaptic plasticity is the major focus of many neuroscientists. There are two major reasons for searching new genes and molecules contributing to central plasticity: first, it provides basic neural mechanism for learning and memory, a key function of the brain; second, it provides new targets for treating brain-related disease. Here, I propose that LTP in the anterior cingulate cortex (ACC) as a synaptic model for emotional fear and chronic pain in the brain. Integrative approaches including genetic, neurobiological and physiological methods are used to investigate the roles of cortical neurons and microglia in synaptic LTP, fear and chronic pain. We have identified several key calcium-stimulated signaling molecules including AC1, CaMKIV and FMRP for AMPA receptor mediated cingulate LTP, trace fear memory, and chronic pain. By contrast, microglia only contributes to changes in spinal dorsal horn, but not in the cortex. Our findings strongly suggest that ACC LTP may serve as a cellular model for studying central sensitization that related to fear and chronic pain, as well as pain-related cognitive emotional disorders.

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Synaptic Plasticity and its Modulation by Alcohol

Brain Plasticity ◽

10.3233/bpl-190089 ◽

2020 ◽

Vol 6 (1) ◽

pp. 103-111 ◽

Cited By ~ 2

Author(s):

Yosef Avchalumov ◽

Chitra D. Mandyam

Keyword(s):

Synaptic Plasticity ◽

Learning And Memory ◽

Dorsal Striatum ◽

Long Term Potentiation ◽

Brain Regions ◽

Public Health Issue ◽

Cellular Mechanisms ◽

Brain Disorder ◽

The Brain

Alcohol is one of the oldest pharmacological agents used for its sedative/hypnotic effects, and alcohol abuse and alcohol use disorder (AUD) continues to be major public health issue. AUD is strongly indicated to be a brain disorder, and the molecular and cellular mechanism/s by which alcohol produces its effects in the brain are only now beginning to be understood. In the brain, synaptic plasticity or strengthening or weakening of synapses, can be enhanced or reduced by a variety of stimulation paradigms. Synaptic plasticity is thought to be responsible for important processes involved in the cellular mechanisms of learning and memory. Long-term potentiation (LTP) is a form of synaptic plasticity, and occurs via N-methyl-D-aspartate type glutamate receptor (NMDAR or GluN) dependent and independent mechanisms. In particular, NMDARs are a major target of alcohol, and are implicated in different types of learning and memory. Therefore, understanding the effect of alcohol on synaptic plasticity and transmission mediated by glutamatergic signaling is becoming important, and this will help us understand the significant contribution of the glutamatergic system in AUD. In the first part of this review, we will briefly discuss the mechanisms underlying long term synaptic plasticity in the dorsal striatum, neocortex and the hippocampus. In the second part we will discuss how alcohol (ethanol, EtOH) can modulate long term synaptic plasticity in these three brain regions, mainly from neurophysiological and electrophysiological studies. Taken together, understanding the mechanism(s) underlying alcohol induced changes in brain function may lead to the development of more effective therapeutic agents to reduce AUDs.

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Molecular and cellular mechanisms underlying brain metastasis of breast cancer

Cancer and Metastasis Reviews ◽

10.1007/s10555-020-09881-y ◽

2020 ◽

Vol 39 (3) ◽

pp. 711-720 ◽

Cited By ~ 2

Author(s):

Mari Hosonaga ◽

Hideyuki Saya ◽

Yoshimi Arima

Keyword(s):

Breast Cancer ◽

Brain Metastasis ◽

Brain Metastases ◽

Cancer Cells ◽

Metastatic Cancer ◽

Breast Cancer Patients ◽

Cellular Mechanisms ◽

Her2 Positive ◽

Cells Of The Microenvironment ◽

The Brain

Abstract Metastasis of cancer cells to the brain occurs frequently in patients with certain subtypes of breast cancer. In particular, patients with HER2-positive or triple-negative breast cancer are at high risk for the development of brain metastases. Despite recent advances in the treatment of primary breast tumors, the prognosis of breast cancer patients with brain metastases remains poor. A better understanding of the molecular and cellular mechanisms underlying brain metastasis might be expected to lead to improvements in the overall survival rate for these patients. Recent studies have revealed complex interactions between metastatic cancer cells and their microenvironment in the brain. Such interactions result in the activation of various signaling pathways related to metastasis in both cancer cells and cells of the microenvironment including astrocytes and microglia. In this review, we focus on such interactions and on their role both in the metastatic process and as potential targets for therapeutic intervention.

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