Dibenzocyclooctadiene lignans from <i>Schisandra chinensis</i> protect primary cultures of rat cortical cells from glutamate‐induced toxicity

Kim, So Ra; Lee, Mi Kyeong; Koo, Kyung Ah; Kim, Seung Hyun; Sung, Sang Hyun; Lee, Na Gyong; Markelonis, George J.; Oh, Tae Hwan; Yang, Jihoon; Kim, Young Choong

doi:10.1002/jnr.20089

Cited by 100 publications

(67 citation statements)

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“…Structural integrity as indicated by the decrease in sensitivity to Ca 2+ stimulated mitochondrial permeability transition in-vitro, was further evidenced by decrease in the extents of mitochondrial malondialdehyde (MDA) production, Ca 2+ loading, and cytochrome c release (Chen, Chiu et al 2008). Sch B also shown to have protection against L-glutamate induced neurotoxicity and the protection was associated with 1) an inhibition of the increase of intracellular [Ca 2+ ]; 2) an improvement in the glutathione defense system, the level of glutathione, and the activity of glutathione peroxidase (GPx); and 3) an inhibition in the formation of cellular peroxide (Kim, Lee et al 2004). Recently Sch B was reported to have protection against amyloid beta and homocysteine induced neurotoxicity in PC12 in-vitro system (Song, Lin et al;Wang and Wang 2009).…”

Section: Neuroprotective Potential Of Sch Bmentioning

confidence: 99%

Schisandrin B, a Lignan from Schisandra chinensis Prevents Cerebral Oxidative Damage and Memory Decline Through Its Antioxidant Property

Konishi¹,

Giridharan²,

Thandavarayan³

2012

When Things Go Wrong - Diseases and Disorders of the Human Brain

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Section: Neuroprotective Potential Of Sch Bmentioning

confidence: 99%

Schisandrin B, a Lignan from Schisandra chinensis Prevents Cerebral Oxidative Damage and Memory Decline Through Its Antioxidant Property

Konishi¹,

Giridharan²,

Thandavarayan³

2012

When Things Go Wrong - Diseases and Disorders of the Human Brain

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“…This study attempts to treat epilepsy by stabilizing the intra-synaptic actin skeleton Schisandra is a traditional Chinese medicine, which play roles in central inhibition and the role of tranquilization [15]. Studies have shown that schizandrine can prevent glutamate induced neuronal damage and antioxidation [10][11]. It not only effectively prevents the damage of the oxidative stress induced by glutamate in the rat brain, but also improves the memory function of mice by regulating the level of acetylcholine.…”

Section: Introductionmentioning

confidence: 99%

Effect of schizandra B on reorganization of primary hippocampus neurons dendritic spine induced by epilepsy

Song¹,

Wang²,

Chen³

2018

Proceedings of the 2018 7th International Conference on Energy, Environment and Sustainable Development (ICEESD 2018)

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Abstract:To investigate the effect of schizandra B(Sch B) on reorganization of primary hippocampus cells dendritic spines induced by Glu. Methods: The primary hippocampus cells were divided into control group, model group and Sch B group. The primary cells in control group were untreated; the primary cells in model group were treated with Glu(15mmol.L-1)for 24h. The primary cells in Sch B group were firstly pretreated with Sch B （0.5μmmol.L-1） for 2h, and exposed to Glu(15mmol.L-1)for 24h. Results: A significant decrease of spines in number was found in the model group cells（3± 2.0/ 10μm n=12） when compared whose those in the control（12± 3.0/μm n=10，p<0.01,t-test）. A slightly decrease of spines in number were found in cells of Sch B group (8± 2.0/ 10μm n=12). Western blot analysis revealed that there is no effect on the total levels of actin and cofilin; However, it can decrease the levels of p-cofilin in the model group. The levels of p-cofilin in Sch B Group is higher than those in model group. Conclusion: Sch B can protect the damage of dendritic spines caused by Glu that is related to inhibit the activation of p-cofilin.Patients with epilepsy often have cognitive impairment due to epilepsy itself [1][2][3][4]. Seizures can cause mild changes in dendritic morphology and dendritic spine of neurons. Dendritic spines is neuronal excitatory postsynaptic component. The number of dendritic spines of hippocampus and neocortex that is related to memory and cognition were decreased in the patient of epilepsy. We hypothesis abnormal dendritic spines maybe causes cognitive damage. [5][6].The changes of the cytokines skeleton changes in glutamate activation are related to the seizure. Glutamate antagonist can prevent the decrease number of dendritic spines caused by seizures. Glutamate agonists kainic acid induced seizures cause the decrease in the number of dendritic spines in hippocampal CA1 area and the neocortex, which is caused by depolymerization of actin cytoskeleton cofilin [14]. At present, epilepsy is mainly controlled by antagonism of neurotransmitters or by blocking ion channels. This study attempts to treat epilepsy by stabilizing the intra-synaptic actin skeleton Schisandra is a traditional Chinese medicine, which play roles in central inhibition and the role of tranquilization [15]. Studies have shown that schizandrine can prevent glutamate induced neuronal damage and antioxidation [10][11]. It not only effectively prevents the damage of the oxidative stress induced by glutamate in the rat brain, but also improves the memory function of mice by regulating the level of acetylcholine. It also promoted dendritic growth and synaptic formation in

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“…There are several reports on the advantages of gomisins A, G, and J. Gomisin A protects the liver by blocking the metabolism of harmful chemicals by inhibiting cytochrome P450-3A4; 16 it also protects against neurotoxicity. 17 Gomisin G's anti-human immunodeficiency virus effects occur via the inhibition of human immunodeficiency virus type 1 reverse transcriptase. 18 Gomisin J has antioxidative effects in myoblast cells 19 and suppresses inflammatory responses.…”

Section: Introduction Imentioning

confidence: 99%

Anti-Inflammatory Effect of Heme Oxygenase-1 TowardPorphyromonas gingivalisLipopolysaccharide in Macrophages Exposed to Gomisins A, G, and J

Ryu

Park

Kim

et al. 2011

Journal of Medicinal Food

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Periodontitis, a chronic inflammatory periodontal disease that develops from gingivitis, is caused by periodontal pathogenic bacteria such as Porphyromonas gingivalis. Recent studies have focused on the antioxidant, anti-human immunodeficiency virus, anticarcinogenic, and anti-inflammatory properties of gomisins. However, the anti-inflammatory activities of gomisin plants through heme oxygenase-1 (HO-1) signals remain poorly defined. We found that gomisins' antiinflammatory activity occurs via the induction of HO-1 expression. Gomisins G and J inhibit the production of the proinflammatory cytokines tumor necrosis factor-a, interleukin-1b, and interleukin-6 and also block nuclear factor-jB activation in Raw264.7 cells stimulated with P. gingivalis lipopolysaccharide. Furthermore, pro-inflammatory cytokine production is inhibited through the induction of HO-1 expression. HO-1 expression is induced by all gomisins, but their anti-inflammatory activity via HO-1 signaling is observed with gomisins G and J, and not A. We found that gomisins G and J extracted from Schisandria chinensis can inhibit the P. gingivalis lipopolysaccharide induced-inflammatory responses in Raw264.7 cells.KEY WORDS: gomisins A, G, and J heme oxygenase-1 nuclear factor E2-related factor 2 Porphyromonas gingivalis lipopolysaccharide pro-inflammatory cytokines

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Dibenzocyclooctadiene lignans from Schisandra chinensis protect primary cultures of rat cortical cells from glutamate‐induced toxicity

Cited by 100 publications

References 50 publications

Schisandrin B, a Lignan from Schisandra chinensis Prevents Cerebral Oxidative Damage and Memory Decline Through Its Antioxidant Property

Schisandrin B, a Lignan from Schisandra chinensis Prevents Cerebral Oxidative Damage and Memory Decline Through Its Antioxidant Property

Effect of schizandra B on reorganization of primary hippocampus neurons dendritic spine induced by epilepsy

Anti-Inflammatory Effect of Heme Oxygenase-1 TowardPorphyromonas gingivalisLipopolysaccharide in Macrophages Exposed to Gomisins A, G, and J

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