针刺抑制p53mRNA过表达并改善SAMP8小鼠的认知能力

[目的]探讨针刺延缓脑衰老的机制。[方法]将快速老化痴呆小鼠(SAMP8)及其正常同源对照小鼠(SAMR1)分为SAMR1对照组、SAMP8对照组、SAMP8针刺组和SAMP8非穴组。针刺组给予"益气调血,扶本培元"针法治疗;非穴组针刺双胁下两个固定非穴位点;其余两组给予等量的捉抓刺激;每天1次,持续15 d。采用Morris水迷宫测定动物的学习记忆能力;逆转录-聚合酶链反应(RT-PCR)法测定海马p53mRNA表达。[结果]与SAMR1对照组相比,SAMP8各组的学习能力及记忆保持能力出现明显损伤,表现为思维僵化、学习过程减慢;其海马p53mRNA表达明显升高。针刺明显改善SAMP8的认知能力,并降低海马p53mRNA表达,甚至低于正常组。[结论]SAMP8的认知损害与p53基因表达异常有关,针刺通过调节p53mRNA表达延缓SAMP8脑衰老的进程,是针刺改善衰老后认知能力下降的原因之一。

ISCHEMIC PRECONDITIONING RELIEVES ISCHEMIA/REPERFUSION INJURY OF HIPPOCAMPUS NEURONS IN RAT BY INHIBITING p53 AND BAX EXPRESSIONS

Objective To examine whether ischemic preconditioning (IPC) can protect neuron against delayed death in CA1 subfield of hippocampus following reperfusion of a lethal ischemia in rats, and explore the role of p53 and bax in this process. Methods We examined the effect of IPC on delayed neuron death, neuron apoptosis, expressions of p53 and bax gene in the CA1 area of hippocampus in the rats using HE staining, flow cytometry, RT-PCR, and immunohistochemistry technique. Results IPC enhanced the quantity of survival cells in the CA1 region of hippocampus (216±9 cells/0.72 mm2 vs. 30±5 cells/0.72 mm2, P<0.01), decreased the percentages of apoptotic neurons of hippocampus caused by ischemia/reperfusion (2.06%±0.21% vs. 4.27%±0.08%, P<0.01), and weakened the expressions of p53 and bax gene of hippocampus compared with ischemia/reperfusion without IPC. Conclusion IPC can protect the neurons in the CA1 region of hippocampus against apoptosis caused by ische- mia/reperfusion, and this process may be related to the reduced expressions of p53 and bax.