基础医学与临床 ›› 2016, Vol. 36 ›› Issue (4): 456-461.

• 研究论文 • 上一篇    下一篇

缺血性脑卒中小鼠脑和血清中IL-17A的变化及其对缺血神经元的影响

于津泠1,李淑娟2,魏海萍1,朱弘倚1,韩松3,李俊发4   

  1. 1. 首都医科大学基础医学院神经生物学系
    2. 首都医科大学附属朝阳医院
    3. 首都医科大学神经生物学系
    4. 首都医科大学
  • 收稿日期:2015-09-28 修回日期:2016-01-16 出版日期:2016-04-05 发布日期:2016-03-29
  • 通讯作者: 李俊发 E-mail:junfali@ccmu.edu.cn
  • 基金资助:
    蛋白激酶Cgamma在缺血性卒中鼠脑皮层神经元缺血损伤中作用及其分子机制研究;缺血性脑卒中内源性神经保护机制和干预措施及生物分子标记物研究;差异表达miRNA对脑缺血/低氧损伤后蛋白激酶C亚型表达的影响及其脑保护作用;缺血/低氧预适应脑内特定miRNAs-PKC 亚型特异性信号通路生物学验证及其抗脑缺血/低氧损伤作用

Changes of IL-17A in brain and serum and its effect on ischemic neurons of mice with ischemic stroke

  • Received:2015-09-28 Revised:2016-01-16 Online:2016-04-05 Published:2016-03-29
  • Contact: Jun-fa LI E-mail:junfali@ccmu.edu.cn

摘要: 目的 观察白介素-17A(IL-17A)在小鼠缺血性脑卒中血清和脑脊液的变化。在离体氧糖剥夺(OGD)模型和基因敲除小鼠中,进一步探讨IL-17A在神经元缺血损伤中可能的作用及其损伤途径。 方法 建立小鼠大脑中动脉栓塞(MCAO)和脑皮层原代神经元氧糖剥夺(OGD)模型,用酶联免疫吸附试验(ELISA)分别检测6及12 h和1、3及7 d的血清(n=7)、脑脊液和12 h梗死区周围皮层(n=5)IL-17A的含量,经5、10、100和500 ng/mL重组IL-17A(rIL-17A)处理后的野生小鼠(n=8)与未经rIL-17A处理的基因敲除小鼠原代神经元进行OGD(n=5),用MTS比色法和蛋白印迹方法检测其对缺血神经元的影响。 结果 MCAO 1 h再灌12 h,梗死区周围脑皮层匀浆IL-17A升高(P<0.001),脑脊液中IL-17A在12 h达到高峰(P<0.05);MCAO 1 h再灌1 d,血清IL-17A开始升高,再灌3 d达到高峰(P<0.001);rIL-17A对常氧下神经元的存活率无明显影响,但其可呈剂量依赖性明显加重OGD损伤后神经元的存活率(P<0.05);OGD处理野生型(IL-17A+/+)小鼠脑皮层原代神经元,Beclin 1蛋白表达水平和Cl/pro-caspase 3的比值明显升高,缺乏IL-17A可以逆转OGD的作用(P<0.05)。 结论 缺血性脑卒中小鼠的血清和脑脊液中IL-17A呈现不同的变化规律,IL-17A可能通过神经元的自噬和凋亡途径加重神经元缺血损伤。

关键词: 白介素-17A(IL-17A),缺血性脑卒中,血清,脑脊液(CSF),氧糖剥夺(OGD), 小鼠

Abstract: Objective To explore the changes of interleukin -17A(IL-17A)in cerebrospinal fluid(CSF) and serum after ischemic stroke. And then investigate its role in ischemic neuronal injury and its possible pathway. Methods Establish mouse cerebral artery occlusion (MCAO) model and oxygen-glucose deprivation (OGD) model with cortical primary neurons, and use enzyme-linked immunosorbent assay (ELISA) to detect the level of IL-17A in serum and cerebrospinal fluid at 6, 12 h, 1, 3, 7 d and per-infarct cortex homogenates at 12 h. With 5, 10, 100 and 500 ng / mL of recombinant IL-17A (rIL-17A) and OGD treatment on wild-type mice (n = 8) and without rIL-17A treatment on knockout mice (n = 5), use MTS assay and Western Blot to detect its effect on ischemic neurons. Results IL-17A significately increased in per-infarct cortex homogenates(P<0.001, n=5) and CSF at 12 h after MCAO (P<0.05, n=5), while in serum it began to increase at 1 d(P<0.05, n=5) and peaked at 3 d (P<0.001, n=7); In vitro, rIL-17A aggravated neuronal death in dose-dependent manner after OGD while it had no effect on neuronal death under normoxia culture(P<0.05,n=8); The ratio of Cl/pro-caspase 3 and the Beclin 1 protein levels increased after OGD treatment. However, this effect could be reversed in lacking of IL-17A after OGD treatment (P<0.05, n=5). Conclusion IL-17A in the serum and CSF after ischemic stroke show different change, and it plays an important role in aggravating neuronal injury possibly through autophagy and apoptosis pathways.

Key words: Interleukin-17A, Ischemic stroke, Serum, Cerebrospinal fluid (CSF), Oxygen-glucose deprivation (OGD), Mice

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