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首页> 外文期刊>Life sciences >NADPH-d and Fos reactivity in the rat spinal cord following experimental spinal cord injury and embryonic neural stem cell transplantation.
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NADPH-d and Fos reactivity in the rat spinal cord following experimental spinal cord injury and embryonic neural stem cell transplantation.

机译:实验性脊髓损伤和胚胎神经干细胞移植后,大鼠脊髓中的NADPH-d和Fos反应性。

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AIMS: The aim of this study is to determine the role of nitric oxide (NO) in neuropathic pain and the effect of embryonic neural stem cell (ENSC) transplantation on NO content in rat spinal cord neurons following spinal cord injury (SCI). MAIN METHODS: Ninety adult male Sprague-Dawley rats were divided into 3 groups (n=30, each): control (laminectomy), SCI (hemisection at T12-T13 segments) and SCI+ENSC. Each group was further divided into sub-groups (n=5 each) based on the treatment substance (L-NAME, 75 mg/kg/i.p.; L-arginine, 225 mg/kg/i.p.; physiological saline, SF) and duration (2h for acute and 28 days for chronic groups). Pain was assessed by tail flick and Randall-Selitto tests. Fos immunohistochemistry and NADPH-d histochemistry were performed in segments 2 cm rostral and caudal to SCI. KEY FINDINGS: Tail-flick latency time increased in both acute and chronic L-NAME groups and increased in acute and decreased in chronic L-arginine groups. The number of Fos (+) neurons decreased in acute and chronic L-NAME and decreased in acute L-arginine groups. Following ENSC, Fos (+) neurons did not change in acute L-NAME but decreased in the chronic L-NAME groups, and decreased in both acute and chronic L-arginine groups. NADPH-d (+) neurons decreased in acute L-NAME and increased in L-arginine groups with and without ENSC transplantation. SIGNIFICANCE: This study confirms the role of NO in neuropathic pain and shows an improvement following ENSC transplantation in the acute phase, observed as a decrease in Fos(+) and NADPH-d (+) neurons in spinal cord segments rostral and caudal to injury.
机译:目的:本研究的目的是确定一氧化氮(NO)在神经性疼痛中的作用以及胚胎神经干细胞(ENSC)移植对脊髓损伤(SCI)后大鼠脊髓神经元中NO含量的影响。主要方法:将90只成年雄性Sprague-Dawley大鼠分为3组(每组30只):对照组(椎板切除术),SCI(T12-T13段的半切术)和SCI + ENSC。根据治疗物质(L-NAME,75 mg / kg / ip; L-精氨酸,225 mg / kg / ip;生理盐水,SF)和持续时间,将每组进一步分为亚组(每组n = 5) (急性组为2h,慢性组为28天)。通过甩尾和Randall-Selitto测试评估疼痛。 Fos免疫组织化学和NADPH-d组织化学在SCI的头侧和尾部2 cm处进行。主要发现:甩尾潜伏时间在急性和慢性L-NAME组中均增加,在急性L-NAME组中增加,而在慢性L-精氨酸组中减少。在急性和慢性L-NAME中,Fos(+)神经元的数量减少,而在急性L-精氨酸组中则减少。在ENSC之后,Fos(+)神经元在急性L-NAME组中没有变化,但在慢性L-NAME组中下降,而在急性和慢性L-精氨酸组中均下降。有和没有ENSC移植的急性L-NAME中,NADPH-d(+)神经元减少,而L-精氨酸组中增加。意义:这项研究证实了NO在神经性疼痛中的作用,并显示了急性期ENSC移植后NO的改善,观察到脊髓前部和尾部脊髓节段的Fos(+)和NADPH-d(+)神经元减少。

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