The roles of P2X7 receptor in regional-specific microglial responses in the rat brain following status epilepticus

Choi, Hea Kyung; Ryu, Hea Jin; Kim, Jieun; Jo, Seung-Mook; Choi, Hojun; Song, Hong-Ki; Kang, Tae‐Cheon

doi:10.1007/s10072-011-0740-z

Cited by 18 publications

(18 citation statements)

References 54 publications

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“…Activation of the pore-forming function of the P2X 7 R was also found to be required for microglial proliferation (Monif et al, 2009). Consistent with this model, blockade of P2X 7 R reduces microglia activation after status epilepticus (Kim et al, 2009; Choi et al, 2012; Engel et al, 2012a). Targeting the pore-forming functions of the P2X 7 R may therefore be a novel approach to limit microglia responses following status epilepticus.…”

Section: Glia-related Functions Of the P2x7r In Status Epilepticusmentioning

confidence: 63%

“…KA, intra-peritoneal KA; Pilo, Pilocarpine; i.p. Pic, intra-peritoneal Picrotoxin; IgG-P2X 7 , anti-P2X 7 antibodies; Il-1β, interleukin-1beta; qPCR, quantitative polymerase chain reaction; IH, Immunohistochemistry; TNF-α, Tumor necrosis factor alpha; W, Western blot .aCavaliere et al, 2007;bLalo et al, 2008;cEngel et al, 2012a;dAvignone et al, 2008;eKanjhan et al, 1999;fRubio and Soto, 2001;gDona et al, 2009;hSeguela et al, 1996;iCollo et al, 1996;jLe et al, 1998;kUlmann et al, 2013;lGuo et al, 2008;mArmstrong et al, 2002;nYu et al, 2008;oJimenez-Pacheco et al, 2013;pRappold et al, 2006;qKim and Kang, 2011;rChoi et al, 2012;sKim et al, 2011a;t Kim et al, 2011b .…”

Section: Expressional Response Of P2x Receptors Following Status Epilmentioning

confidence: 99%

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P2X receptors as targets for the treatment of status epilepticus

Henshall

Dı́az-Hernández

Miras‐Portugal

et al. 2013

Front. Cell. Neurosci.

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Prolonged seizures are amongst the most common neurological emergencies. Status epilepticus is a state of continuous seizures that is life-threatening and prompt termination of status epilepticus is critical to protect the brain from permanent damage. Frontline treatment comprises parenteral administration of anticonvulsants such as lorazepam that facilitate γ-amino butyric acid (GABA) transmission. Because status epilepticus can become refractory to anticonvulsants in a significant proportion of patients, drugs which act on different neurotransmitter systems may represent potential adjunctive treatments. P2X receptors are a class of ligand-gated ion channel activated by ATP that contributes to neuro- and glio-transmission. P2X receptors are expressed by both neurons and glia in various brain regions, including the hippocampus. Electrophysiology, pharmacology and genetic studies suggest certain P2X receptors are activated during pathologic brain activity. Expression of several members of the family including P2X2, P2X4, and P2X7 receptors has been reported to be altered in the hippocampus following status epilepticus. Recent studies have shown that ligands of the P2X7 receptor can have potent effects on seizure severity during status epilepticus and mice lacking this receptor display altered seizures in response to chemoconvulsants. Antagonists of the P2X7 receptor also modulate neuronal death, microglial responses and neuroinflammatory signaling. Recent work also found altered neuronal injury and inflammation after status epilepticus in mice lacking the P2X4 receptor. In summary, members of the P2X receptor family may serve important roles in the pathophysiology of status epilepticus and represent novel targets for seizure control and neuroprotection.

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Section: Glia-related Functions Of the P2x7r In Status Epilepticusmentioning

confidence: 63%

Section: Expressional Response Of P2x Receptors Following Status Epilmentioning

confidence: 99%

P2X receptors as targets for the treatment of status epilepticus

Henshall

Dı́az-Hernández

Miras‐Portugal

et al. 2013

Front. Cell. Neurosci.

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“…Previous studies have shown that P2X7R antagonists trigger anticonvulsant effect, reducing electrographic and behavioral seizures, microglia activation, decrease IL-1β production and prevent cell damage resulting from seizures [14,15,33,38,41,42]. Studies using P2X7R (Pfizer) [46] knockout mice also show reduction in the severity of seizures compared to wild-type mice [33].…”

Section: Discussionmentioning

confidence: 84%

“…There are many studies aimed at elucidating the role of P2X7R in epilepsy using agonists and antagonists. The activation of P2X7R with Bz-ATP (P2X7R agonist) causes microglial activation, enhances TNF-α immunoreactivity, reduces astrocytes, and intensifies seizures expression [19,[38][39][40]. Conversely, P2X7R blockage promotes anticonvulsant effects and reduces electroencephalographic and behavioral seizures, IL-1β production, microglial activation, recruitment and infiltration of neutrophils into the frontoparietal cortex, and damage resulting from seizure [14,15,33,38,[41][42][43][44].…”

Section: Introductionmentioning

confidence: 99%

“…The activation of P2X7R with Bz-ATP (P2X7R agonist) causes microglial activation, enhances TNF-α immunoreactivity, reduces astrocytes, and intensifies seizures expression [19,[38][39][40]. Conversely, P2X7R blockage promotes anticonvulsant effects and reduces electroencephalographic and behavioral seizures, IL-1β production, microglial activation, recruitment and infiltration of neutrophils into the frontoparietal cortex, and damage resulting from seizure [14,15,33,38,[41][42][43][44]. Surprisingly, P2X7R antagonists have been described to exacerbate seizures and enhance cell death in the hippocampal CA3 subfield in the pilocarpine and intraamygdala kainic acid models, but do not change behavioral pattern in the intraperitoneal kainic acid and picrotoxin models of epilepsy [39,41,45].…”

Section: Introductionmentioning

confidence: 99%

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Silencing of P2X7R by RNA interference in the hippocampus can attenuate morphological and behavioral impact of pilocarpine-induced epilepsy

Amorim

Araújo

Valero

et al. 2017

Purinergic Signalling

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Cell signaling mediated by P2X7 receptors (P2X7R) has been suggested to be involved in epileptogenesis, via modulation of intracellular calcium levels, excitotoxicity, activation of inflammatory cascades, and cell death, among other mechanisms. These processes have been described to be involved in pilocarpine-induced status epilepticus (SE) and contribute to hyperexcitability, resulting in spontaneous and recurrent seizures. Here, we aimed to investigate the role of P2X7R in epileptogenesis in vivo using RNA interference (RNAi) to inhibit the expression of this receptor. Small interfering RNA (siRNA) targeting P2X7R mRNA was injected into the lateral ventricles (icv) 6 h after SE. Four groups were studied: SalineVehicle, Saline-siRNA, Pilo-Vehicle, and Pilo-siRNA. P2X7R was quantified by western blotting and neuronal death assessed by Fluoro-Jade B histochemistry. The hippocampal volume (edema) was determined 48 h following RNAi. Behavioral parameters as latency to the appearance of spontaneous seizures and the number of seizures were determined until 60 days after the SE onset. The Saline-siRNA and Pilo-siRNA groups showed a 43 and 37% reduction, respectively, in P2X7R protein levels compared to respective vehicle groups. Neuroprotection was observed in CA1 and CA3 of the PilosiRNA group compared to Pilo-Vehicle. P2X7R silencing in pilocarpine group reversed the increase in the edema detected in the hilus, suprapyramidal dentate gyrus, CA1, and CA3; reduced mortality rate following SE; increased the time to onset of spontaneous seizure; and reduced the number of seizures, when compared to the Pilo-Vehicle group. Therefore, our data highlights the potential of P2X7R as a therapeutic target for the adjunct treatment of epilepsy.

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Development and sensory experience dependent regulation of microglia in barrel cortex

Kalambogias

Chen

Khan

et al. 2019

J of Comparative Neurology

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The barrel cortex is within the primary somatosensory cortex of the rodent, and processes signals from the vibrissae. Much focus has been devoted to the function of neurons, more recently, the role of glial cells in the processing of sensory input has gained increasing interest. Microglia are the principal immune cells of the nervous system that survey and regulate the cellular constituents of the dynamic nervous system. We investigated the normal and disrupted development of microglia in barrel cortex by chronically depriving sensory signals via whisker trimming for the animals’ first postnatal month. Using immunohistochemistry to label microglia, we performed morphological reconstructions as well as densitometry analyses as a function of developmental age and sensory experience. Findings suggest that both developmental age and sensory experience has profound impact on microglia morphology. Following chronic sensory deprivation, microglia undergo a morphological transition from a monitoring or resting state to an altered morphological state, by exhibiting expanded cell body size and retracted processes. Sensory restoration via whisker regrowth returns these morphological alterations back to age‐matched control values. Our results indicate that microglia may be recruited to participate in the modulation of neuronal structural remodeling during developmental critical periods and in response to alteration in sensory input.

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The roles of P2X7 receptor in regional-specific microglial responses in the rat brain following status epilepticus

Cited by 18 publications

References 54 publications

P2X receptors as targets for the treatment of status epilepticus

P2X receptors as targets for the treatment of status epilepticus

Silencing of P2X7R by RNA interference in the hippocampus can attenuate morphological and behavioral impact of pilocarpine-induced epilepsy

Development and sensory experience dependent regulation of microglia in barrel cortex

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