Vinpocetine halts ketamine-induced schizophrenia-like deficits in rats: impact on BDNF and GSK-3β/β-catenin pathway

Ahmed, Hebatalla I.; Abdel-Sattar, Somaia A.; Zaky, Heba S.

doi:10.1007/s00210-018-1552-y

Cited by 27 publications

(24 citation statements)

References 81 publications

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“…These events lead to reduction of cAMP system which is important in the expression and regulation of brain derived neurotrophic factor (BDNF), which improves neuronal survival. PDE1 is mainly localized in striatum and cortex which participating in the regulation of neuronal motor activity [17,18].…”

Section: Vinpocetine In Ischemic Strokementioning

confidence: 99%

Vinpocetine and Ischemic Stroke

Al-Kuraishy¹,

Al-Gareeb²

2021

Ischemic Stroke

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Vinpocetine (VPN) is a synthetic ethyl-ester derivative of the alkaloid apovincamine from Vinca minor leaves. VPN is a selective inhibitor of phosphodiesterase type 1 (PDE1) has potential neurological effects through inhibition of voltage gated sodium channel and reduction of neuronal calcium influx. VPN have noteworthy antioxidant, anti-inflammatory and anti-apoptotic effects with inhibitory effect on glial and astrocyte cells during and following ischemic stroke (IS). VPN is effective as an adjuvant therapy in the management of epilepsy; it reduces seizure frequency by 50% in a dose of 2 mg/kg/day. VPN improves psychomotor performances through modulation of brain monoamine pathway mainly on dopamine and serotonin, which play an integral role in attenuation of depressive symptoms. VPN recover cognitive functions and spatial memory through inhibition of hippocampal and cortical PDE-1with augmentation of cAMP/cGMP ratio, enhancement of cholinergic neurotransmission and inhibition of neuronal inflammatory mediators. Therefore, VPN is an effective agent in the management of ischemic stroke and plays an integral role in the prevention and attenuation of post-stroke epilepsy, depression and cognitive deficit through direct cAMP/cGMP-dependent pathway or indirectly through anti-inflammatory and anti-oxidant effects.

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Section: Vinpocetine In Ischemic Strokementioning

confidence: 99%

Vinpocetine and Ischemic Stroke

Al-Kuraishy¹,

Al-Gareeb²

2021

Ischemic Stroke

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“…PDE1 is mainly localized in striatum and cortex which participating in the regulation of neuronal motor activity. [17,18] Indeed, VPN increases neuronal cGMP through inhibition of calmodulin-dependent phosphodiesterase which improves cerebral blood flow and oxygen consumption. [19] VPN improves cerebral metabolism through enhancing glucose and oxygen supply and ATP production by cerebral vasodilation.…”

Section: Pharmacology Of Vinpocetinementioning

confidence: 99%

Role of vinpocetine in ischemic stroke and poststroke outcomes: A critical review

et al. 2020

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Vinpocetine (VPN) is a synthetic ethyl-ester derivative of the alkaloid apovincamine from Vinca minor leaves. VPN is a selective inhibitor of phosphodiesterase type 1 (PDE1) that has potential neurological effects through inhibition of voltage-gated sodium channel and reduction of neuronal calcium influx. VPN has noteworthy antioxidant, anti-inflammatory, and anti-apoptotic effects with inhibitory effect on glial and astrocyte cells during and following ischemic stroke (IS). VPN is effective as adjuvant therapy in the management of epilepsy; it reduces seizure frequency by 50% in a dose of 2 mg/kg/day. VPN improves psychomotor performances through modulation of brain monoamine pathway mainly on dopamine and serotonin, which play an integral role in attenuation of depressive symptoms. VPN recover cognitive functions and spatial memory through inhibition of hippocampal and cortical PDE1 with augmentation of cyclic adenosin monophosphate and cyclic guanosin monophosphate ratio, enhancement of cholinergic neurotransmission, and inhibition of neuronal inflammatory mediators. Therefore, VPN is an effective agent in the management of IS and plays an integral role in the prevention and attenuation of poststroke epilepsy, depression, and cognitive deficit through direct cAMP/cGMP-dependent pathway or indirectly through anti-inflammatory and antioxidant effects.

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“…Vinpocetine has been shown to correct primary deficits such as social behavior and repetitive behavior in a rodent model of entorhinal cortex lesion (Nyakas et al, 2009). Also, behavioral deficits, such as anxiety, hyperactivity/hyper‐locomotion and nociception were found to be mitigated in murine models of, schizophrenia, attention deficit hyperactivity disorder and inflammatory pain (Abreu‐Villaça et al, 2018; Ahmed et al, 2018; Ruiz‐miyazawa, Pinho‐ribeiro, et al, 2015). Further, PDE1 inhibition is known to ameliorate several neurochemical deficits, such as brain inflammation, brain oxidative stress and neuronal dysfunction, in rodent models of fetal alcohol syndrome, Huntington's disease and early ethanol exposure (Gupta & Sharma, 2014; Krahe et al, 2009; Swart et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Vinpocetine amended prenatal valproic acid induced features of ASD possibly by altering markers of neuronal function, inflammation, and oxidative stress

Luhach

Kulkarni²,

Singh

et al. 2021

Autism Research

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Autism spectrum disorder (ASD) is a neurodevelopmental disorder with complex etiology and phenotypes. Phosphodiesterase-1 (PDE1) inhibitors are known to provide benefits in various brain conditions manifesting similar behavioral phenotypes. The pharmacological consequences of vinpocetine administration a PDE1 inhibitor in prenatal-valproic acid (pre-VPA) induced ASD related behavioral phenotypes (social behavior deficits, repetitive behavior, anxiety, hyperlocomotion, and nociception) was assessed. Also, effects on important biochemical markers of neuronal function (DCX-neurogenesis, BDNF-neuronal survival, synapsin-IIa-synaptic transmission, pCREB-neuronal transcription factor), inflammation (interleukin [IL]-6, IL-10, and TNF-α) and oxidative stress (thiobarbituric acid reactive substance [TBARS] and glutathione (GSH) were studied in important brain areas (frontal cortex, cerebral cortex, hippocampus, and striatum). Further, neuronal cell viability was determined in dentate gyrus using Nissl staining. Pre-VPA administration resulted into impaired behavior, brain biochemistry, and neuronal cell viability. Administration of vinpocetine resulted in improvements of pre-VPA impaired social behavior, repetitive behavior, anxiety, locomotion, and nociception. Also, vinpocetine resulted in a significant increase in the levels of BDNF, synapsin-IIa, DCX, pCREB/CREB, IL-10, and GSH along with significant decrease in TNF-α, IL-6, TBARS, number of pyknotic and chromatolytic cells in different brain areas of pre-VPA group. Finally, high association between behavioral parameters and biochemical parameters was observed upon Pearson's correlation analysis. Vinpocetine, a PDE1 inhibitor rectified important behavioral phenotypes related with ASD, possibly by improving neuronal function, brain inflammation and brain oxidative stress. Thus, PDE1 may be a possible target for further understanding ASD. Lay SummaryASD is a brain developmental disorder with a wide array of genetic and environmental factors. Many targets have been identified till date, but a clinical treatment is still afar. The results of this study indicate that vinpocetine administration resulted in amelioration of ASD associated symptomatology in rats, prenatally exposed to VPA. Our research adds a widely expressed brain enzyme PDE1, as a possible novel pharmacological target and opens-up a new line of enquiry for ASD treatment.

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Vinpocetine halts ketamine-induced schizophrenia-like deficits in rats: impact on BDNF and GSK-3β/β-catenin pathway

Cited by 27 publications

References 81 publications

Vinpocetine and Ischemic Stroke

Vinpocetine and Ischemic Stroke

Role of vinpocetine in ischemic stroke and poststroke outcomes: A critical review

Vinpocetine amended prenatal valproic acid induced features of ASD possibly by altering markers of neuronal function, inflammation, and oxidative stress

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