The Effect of Noscapine on Oxygen-Glucose Deprivation on Primary Murine Cortical Neurons in High Glucose Condition

Authors

  • Nahid Rahbar-Roshandel School of Medicine, Department of Pharmacology, Iran University of Medical Sciences, Tehran, Iran
  • Soltan-Ahmed Ebrahimi School of Medicine, Department of Pharmacology, Iran University of Medical Sciences, Tehran, Iran
Abstract:

AbstractIn the present work we set out to investigate the neuroprotective effects of noscapine (0.5-2 µM) in presence of D-glucose on primary murine foetal cortical neurons after oxygen–glucose deprivation/24 hrs recovery. Cell viability, nitric oxide production and intracellular calcium ([ca2+]i) levels were evaluated by MTT assay, the modified Griess method and Fura-2 respectively. 25 and 100 mM D-glucose could, in a concentration dependent manner, improve cell viability and decrease NO production and [ca2+]i level in neuronal cells after ischemic insult. Moreover, pre-incubation of cells with noscapine, noticeably enhanced protective effects of 25 and 100 mM D-glucose compared to similar conditions without noscapine pre-treatment. In fact, noscapine attenuated NO production in a dose-dependent fashion, after 30 minutes (min) OGD, during high-glucose (HG) condition in cortical neurons. Pretreatment with 2 μM noscapine and 25 or 100 mM D-glucose, was shown to decrease the rise in [ca2+]i induced by Sodium azide/glucose deprivation (chemical OGD) model. These effects were more pronounced than that of 25 or 100 mM D-glucose alone.The present study demonstrated that the neuroprotective effects of HG after an ischemic insult were augmented by pre-treatment with noscapine. Our results also suggested that the neuroprotection offered by both HG and noscapine involve attenuation of NO production and [ca2+]i levels stimulated by the experimental ischemia in cortical neurons.

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the effect of noscapine on oxygen-glucose deprivation on primary murine cortical neurons in high glucose condition

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Journal title

volume 15  issue 2

pages  501- 512

publication date 2016-06-01

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