Anti-Inflammatory Small Molecules To Treat Seizures and Epilepsy: From Bench to Bedside

Dey, Avijit; Xu, Kaiwu; Jiang, Jianxiong; Du, Yifeng

doi:10.1016/j.tips.2016.03.001

Cited by 165 publications

(147 citation statements)

References 172 publications

(203 reference statements)

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“…Today, brain inflammation or neuroinflammation have been associated with many central nervous system (CNS) pathologies (Dey, Kang, Qiu, Du & Jiang 2016). Such processes may have beneficial effects, protecting against exogenous insults or promoting healing, but under certain situations they can be pathogenic.…”

Section: Inflammation and Neuroinflammation: Definitions Targetsmentioning

confidence: 99%

“…Prior studies associated elevated levels of pro-inflammatory cytokines with seizures, the pathogenesis of epilepsy, and pathologies manifesting epilepsy (Table 1) (Vitaliti, Pavone, Mahmood, Nunnari & Falsaperla 2014). Recent studies have introduced the neurological sequelae, in which pro-inflammatory cytokines with proictogenic properties (such as IL-1β, high-mobility group box 1 [HMGB1], cyclooxygenase-2 [COX-2], prostaglandin E2 [PGE2], IL-6, TNF-α and nicotinamide adenine dinucleotide phosphate-oxidase [NOX2]) play an important role in seizure generation and exacerbation (Vezzani, Auvin, Ravizza & Aronica 2012, Wu & Huang 2015, Dey, Kang, Qiu, Du & Jiang 2016). IL-1β and HMGB1 induce the proinflammatory innate immunity IL-1 receptor type 1 (IL-1R1)/toll-like receptor 4 (TLR4) signaling (Ravizza, Kostoula & Vezzani 2013, Vezzani, Lang & Aronica 2016) leading to neuroinflammation, its perpetuation and thus modulating seizure susceptibility, lowering seizure threshold and epileptogenesis (Maroso, Balosso, Ravizza, Liu, Aronica, Iyer et al 2010, Riazi, Galic & Pittman 2010, Vitaliti, Pavone, Mahmood, Nunnari & Falsaperla 2014, Vezzani, Lang & Aronica 2016).…”

Section: Inflammation and Neuroinflammation: Definitions Targetsmentioning

confidence: 99%

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Inflammation in Epileptic Encephalopathies

Shandra

Moshé

Galanopoulou

2017

Stress and Inflammation in Disorders

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West syndrome (WS) is an infantile epileptic encephalopathy (EE) that manifests with infantile spasms, hypsarrhythmia (in ~60% of infants) and poor neurodevelopmental outcomes. The etiologies of WS can be structural-metabolic pathologies (~60%), genetic (12–15%) or of unknown origin. The current treatment options include hormonal treatment [adrenocorticotropic hormone (ACTH) and high dose steroids], the GABA aminotransferase inhibitor vigabatrin, while ketogenic diet can be given as add-on treatment in refractory IS. There is a need to identify new therapeutic targets and more effective treatments for WS. Theories about the role of inflammatory pathways in the pathogenesis and treatment of WS have emerged, being supported by both clinical and preclinical data from animal models of WS. Ongoing advances in genetics have revealed numerous genes involved in the pathogenesis of WS, including genes directly or indirectly involved in inflammation. Inflammatory pathways also interact with other signaling pathways implicated in WS, such as the neuroendocrine pathway. Furthermore, seizures may also activate pro-inflammatory pathways raising the possibility that inflammation can be a consequence of seizures and epileptogenic processes. With this targeted review we plan to discuss the evidence pro and against the following key questions. Does activation of inflammatory pathways in the brain cause epilepsy in WS and does it contribute to the associated comorbidities and progression? Can activation of certain inflammatory pathways be a compensatory or protective event? Are there interactions between inflammation and the neuroendocrine system that contribute to the pathogenesis of West syndrome? Does activation of brain inflammatory signaling pathways contribute to the transition of WS to Lennox-Gastaut syndrome? Are there any lead candidates or unexplored targets for future therapy development for WS targeting inflammation?

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Section: Inflammation and Neuroinflammation: Definitions Targetsmentioning

confidence: 99%

Section: Inflammation and Neuroinflammation: Definitions Targetsmentioning

confidence: 99%

Inflammation in Epileptic Encephalopathies

Shandra

Moshé

Galanopoulou

2017

Stress and Inflammation in Disorders

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“…Development of seizures and epilepsy in animal models and in humans following a variety of brain insults is correlated with neuroinflammation and increased expression of cytokines in brain (18). Cytokines can modulate neurotransmission by affecting the levels of excitatory and inhibitory neurotransmitters and their receptors, enzymes involved in the metabolism of neurotransmitters, and cellular signaling proteins (19).…”

Section: Cytokinesmentioning

confidence: 99%

Novel Targets for Developing Antiseizure and, Potentially, Antiepileptogenic Drugs

2017

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Epilepsy is a devastating neurological disorder affecting nearly 65 million people worldwide. The etiology of epilepsy is heterogeneous in nature and a variety of factors-such as infection, stroke, traumatic brain injury, brain tumors, cerebral ischemia, and importantly, mutations in genes that are crucial for the development, migration, and function of neurons and glia-may cause seizures and lead to the development of epilepsy. Over 25 drugs are clinically available for the symptomatic treatment of the seizures that are the defining criteria of epilepsy. However, most of these drugs tend to optimize the balance between excitatory and inhibitory neurotransmission by modulating the functions of ion channels, receptors, enzymes, and transporters expressed by neurons (1). Importantly, around one-third of epilepsy patients are still pharmacoresistant, and many patients who respond to antiseizure drugs (ASDs) often present with significant adverse effects (2). In addition, people with epilepsy also suffer from co-morbidities such as anxiety, depression, and cognitive impairment. Many ASDs either do not address or, in some instances, aggravate these co-morbidities. Therefore, future ASD development efforts should 1) include novel mechanisms of action for ASDs, 2) evaluate potential therapeutic targets for disease modification, and 3) identify potential therapeutic interventions for the prevention of epilepsy. There are several promising targets for developing novel drugs that might prevent or impede epileptogenesis. Some of these novel targets are discussed in this brief review. Transforming Growth Factor β (TGFβ)Sustained damage to the blood brain barrier (BBB) is associated with increased incidence of seizures (3). Animal studies show that the activation of the TGFβ signaling pathway, mainly in astrocytes by albumin extravasated into brain parenchyma following BBB injury, disrupts regulatory functions of astrocytes and causes hyperexcitability in cortical and limbic structures (4). Direct activation of the TGFβ signaling pathway by TGFβ1 also causes epileptiform activity in rats, whereas TGFβ receptor blockers ameliorate TGFβ1-or albumin-induced epileptiform activity (5). Mice overexpressing TGFβ1 specifically in astrocytes develop seizures (6). It was recently found that losartan, which inhibits TGFβ1 signaling, decreased the number of rats developing albumin-induced chronic spontaneous seizures and inhibited epileptogenesis in this vascular injury-induced model of epilepsy (7). It is evident from these animal studies that inhibition of the TGFβ signaling pathway might be an effective strategy to inhibit seizures and epilepto-

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“…These findings indicate that astrocytic EP3 receptors may be upregulated under pathological conditions, and endothelial PGE 2 may directly activate EP3 receptors on astrocytic end-feet in neurotoxic brain diseases, such as epileptic seizures. PGE 2 also acts on other three receptors, namely EP1, EP2 and EP4, and activation of their receptors has been found to contribute to PGE 2 -mediated neurotoxicity 26 . Block of EP1 receptor reduces proinflammatory responses and neuronal damage in the hippocampus after KA injection in mice 27 .…”

Section: Induction Of Cox-2 and Mpges-1 In The Brainmentioning

confidence: 99%

Endothelial prostaglandin E2 regulates neuronal injury after seizure via activation of astrocytes

Takemiya¹

2017

J Neurol Neuromedicine

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Astrocytes interact closely with neurons via glutamate; this astrocyteneuron circuit may play a pivotal role in synaptic transmission. In addition, astrocytes contact vascular endothelial cells (ECs) with their end-feet; therefore, ECs may have some role in regulating neuronal activity via astrocytes in the brain. In our studies, we found that kainic acid (KA) microinjection induced the expression of microsomal prostaglandin E synthase-1 (mPGES-1) in venous ECs and the expression of the prostaglandin E 2 (PGE 2 ) receptor EP3 on astrocytes. Moreover, endothelial mPGES-1 exacerbated KA-induced neuronal injury in the mouse brain. In in vitro experiments, mPGES-1 produced PGE 2 , which increased astrocytic Ca 2+ levels and Ca 2+ -dependent glutamate release, thus aggravating neuronal injury. We found ECs had a role under pathological conditions and brain ECs are not merely a physiological barrier between the blood and brain; instead, they may also act as a signal transducer or amplifier. Moreover, the endotheliumastrocyte-neuron signaling pathway may be crucial for driving neuronal injury elicited by repetitive seizures and may be a new therapeutic target for epilepsy.

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Anti-Inflammatory Small Molecules To Treat Seizures and Epilepsy: From Bench to Bedside

Cited by 165 publications

References 172 publications

Inflammation in Epileptic Encephalopathies

Inflammation in Epileptic Encephalopathies

Novel Targets for Developing Antiseizure and, Potentially, Antiepileptogenic Drugs

Endothelial prostaglandin E2 regulates neuronal injury after seizure via activation of astrocytes

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