Effect of Alpha and Beta Adrenergic Receptors on the Expression of Stk4, Caspase-3, and Sox2 Genes in Neural Stem Cells Derived From the Hippocampus and Treated With Norepinephrine in Rats

Zakiye Davar, I. Jafari Anarkooli, Mohammadjavad Fridoni, A. Abdanipour
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Abstract

Background and Objectives Uncontrolled stress affects hippocampal-dependent memory through altering the morphology and the proliferation rate of hippocampal progenitor cells. Subjects and Methods In this experimental study, neural stem cells (NSCs) were isolated from the hippocampus of newborn rats and cultivated in a serum-free medium to generate neurosphere. To confirm the induced NSCs, immunocytochemistry and antibody nestin were used. The rate of cell proliferation and cytotoxicity caused by norepinephrine were measured by the MTT assay. NSCs were assigned in the following groups: Control (untreated NSCs), norepinephrine (NSCs treated with norepinephrine), propranolol (NSCs treated with beta receptor blocker propranolol plus norepinephrine), prazosin (NSCs treated with Alfa receptor blocker prazosin plus norepinephrine), and propranolol/ prazosin (NSCs treated with both propranolol and prazosin plus norepinephrine). Real-time PCR was conducted to measure the expression levels of Stk4, Caspase-3 and Sox2 genes. Results The flow cytometry study revealed that NSCs were nestin positive. Real-time PCR results showed that the expression level of Sox2 gene increased by norepinephrine. In addition, the expression level of Stk4 and Caspase-3 genes increased in the groups treated with prazosin. Conclusion The effect of norepinephrine on hippocampus-derived NSCs is receptor-dependent. The increase of norepinephrine under chronic stress can lead to either cell proliferation or apoptosis in NSCs; it acts as a double-edged sword.
α和β肾上腺素受体对大鼠海马神经干细胞Stk4、Caspase-3和Sox2基因表达的影响
背景与目的不受控制的应激通过改变海马祖细胞的形态和增殖速率影响海马依赖记忆。实验对象和方法从新生大鼠海马中分离神经干细胞,在无血清培养基中培养生成神经球。采用免疫细胞化学和抗体巢蛋白法对诱导的NSCs进行验证。用MTT法测定去甲肾上腺素对细胞的增殖率和细胞毒性。将NSCs分为以下组:对照组(未经处理的NSCs)、去甲肾上腺素组(用去甲肾上腺素处理的NSCs)、心得安(用β受体阻滞剂心得安加去甲肾上腺素处理的NSCs)、普拉唑嗪组(用α受体阻滞剂普拉唑嗪加去甲肾上腺素处理的NSCs)、心得安/普拉唑嗪组(用心得安和普拉唑嗪加去甲肾上腺素处理的NSCs)。采用Real-time PCR检测Stk4、Caspase-3和Sox2基因的表达水平。结果流式细胞术显示NSCs为nestin阳性。Real-time PCR结果显示,去甲肾上腺素使Sox2基因表达水平升高。此外,prazosin组Stk4和Caspase-3基因表达水平升高。结论去甲肾上腺素对海马源性NSCs的影响具有受体依赖性。慢性应激下去甲肾上腺素的升高可导致NSCs细胞增殖或凋亡;它就像一把双刃剑。
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