亚低温上调Sirt1减少氧糖剥夺后原代神经元细胞凋亡

尹美娴; 胡春林; 魏红艳; 廖晓星; 李恒杰; 杨焰; 李慧; 荆小莉; 李浩明

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亚低温上调Sirt1减少氧糖剥夺后原代神经元细胞凋亡

论文 | 更新时间：2023-12-11

- 亚低温上调Sirt1减少氧糖剥夺后原代神经元细胞凋亡
- Mild hypothermia reduces neurons apoptosis after OGD by up-regulating Sirt1
- 中山大学学报(自然科学版)(中英文) 2017年56卷第6期页码：134-140
- 作者机构：
  
  1. 广东药科大学生命科学与生物制药学院,广东,广州,510006
  2. 
  3. 中山大学附属第一医院急诊科,广东,广州,510080
- 作者简介：
- 基金信息：
- DOI：
  中图分类号：
- 纸质出版日期：2017，
  
  网络出版日期：2017-11-25，
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尹美娴, 胡春林, 魏红艳, 等. 亚低温上调Sirt1减少氧糖剥夺后原代神经元细胞凋亡[J]. 中山大学学报(自然科学版)(中英文), 2017,56(6):134-140.

YIN Meixian, HU Chunlin, WEI Hongyan, et al. Mild hypothermia reduces neurons apoptosis after OGD by up-regulating Sirt1[J]. Acta Scientiarum Naturalium Universitatis SunYatseni, 2017,56(6):134-140.
尹美娴, 胡春林, 魏红艳, 等. 亚低温上调Sirt1减少氧糖剥夺后原代神经元细胞凋亡[J]. 中山大学学报(自然科学版)(中英文), 2017,56(6):134-140. DOI：

YIN Meixian, HU Chunlin, WEI Hongyan, et al. Mild hypothermia reduces neurons apoptosis after OGD by up-regulating Sirt1[J]. Acta Scientiarum Naturalium Universitatis SunYatseni, 2017,56(6):134-140. DOI：

摘要

为探讨亚低温对氧糖剥夺/复氧后原代神经元细胞自噬和凋亡的影响，运用原代神经元培养及OGD/R模型构建，CCK8测定细胞活力，TUNEL检测细胞凋亡， Westernblot检测Sirt1、Foxo1、Rab7、Beclin1、LC3及p53等蛋白的表达，以及转染mRFP-GFP-LC3自噬双标腺病毒检测神经元自噬流等方法，成功培养原代神经元及构建OGD/R模型。结果发现OGD/R后Sirt1、P-Foxo1、Rab7、Beclin1、LC3b/LC3a表达随着时间延长逐渐减少，12 h更明显，与R6 h组相比，P<0.05

而 p53增加，P<0.05；OGD3 h/R12 h，亚低温组Sirt1、P-Foxo1、Rab7、Beclin1 及 LC3b/LC3a表达均明显高于常温组，P<0.05

而 p53明显低于常温组，P<0.05。R6 h亚低温组，神经元凋亡率为20%±6.7%，低于常温组的56.8%±7.6%，P<0.05。mRFP-GFP-LC3 自噬双标观察法显示亚低温组自噬溶酶体明显增多，P<0.05。实验显示原代神经元OGD/R后亚低温干预可以上调Sirt1的活性，增加Foxo1、Rab7 和自噬相关蛋白Beclin1、LC3b/LC3a的表达，同时抑制p53，促进神经元自噬，减少凋亡。

Abstract

To investigate the primary neurons autophagy and apoptosis after Oxygen Glucose Deprivation/Re-oxygenation (OGD/R)

and to explore the effect of mild hypothermia on autophagy and apoptosis

following methods were used: Primary neurons culture and OGD/R model was established; the neurons were divided into the normal temperature group (37 ℃) and the mild hypothermia group (MH

34 ℃); The cells viability were measured by CCK8; cell apoptosis were measured by TUNEL; The protein expressions of Sirt1

Foxo1

p53

Rab7 and autophagy related genes such as Beclin1

LC3 were detected by western blot at each time point; The neurons autophagy flows were detected through transfection of adenovirus mRFP-GFP-LC3. The primary neuron cultures were successfully developed

and the OGD/R models were established; Westernblot showed that the expressions of Sirt1

P-Foxo1

Rab7

Beclin1 and LC3b/LC3a were gradually reduced

especially at 12 h after OGD/R

P<0.05; However

the expression of p53 was increased

P<0.05; In MH group

the expressions of Sirt1

P-Foxo1

Rab7

Beclin1

LC3b/LC3a were obviously higher than those in NT group

P<0.05; And the expression of p53 was obviously lower than that in NT group

P<0.05; in R6 h+MH group， the rate of neuron cells apoptosis were 20%±6.7%

lower than 56.8%±7.6% in R6 h+NT group

P<0.05; mRFPGFPLC3 adenovirus was transfected into primary neurons

the autophagy flow was detected by fluorescence microscopy. Compared with control group

the autolysosomes were reduced

but autophagosomes were increased after OGD/R

P<0.05; however

compared with NT group

the autophagosomes were reduced and the autolysosomes were increased in MH group

P<0.05. In conclusion

mild hypothermia therapy could increase the expression of Sirt1

Foxo1

beclin1 and LC3b/LC3a

but decrease the expression of p53

so as to promote autophagy and reduce apoptosis.

关键词

亚低温Sirt1神经元细胞

Keywords

mild hypothermiaSirt1neurons

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