文章摘要
陈红媛 王永闯 李立 王莉 俞春江.β-分泌酶抑制剂对tau 过磷酸化大鼠β-CTF代谢的影响及机制研究[J].,2017,17(2):237-241
β-分泌酶抑制剂对tau 过磷酸化大鼠β-CTF代谢的影响及机制研究
The Effects and Mechanisms of β-secretase Inhibitor on the Processing ofβ-CTF in Tau Hyperphosphorylated Rat Model
  
DOI:
中文关键词: 阿尔茨海默病  淀粉样前体蛋白C末端片段  BACE1  tau 过磷酸化
英文关键词: Alzheimer's disease  Amyloid C-terminal fragment of amyloid precursor protein  BACE1  Tau hyperphosphorylation
基金项目:黑龙江省卫生计生委科研基金项目(2014-337);黑龙江省博士后基金项目(LBH-Z15135)
作者单位
陈红媛 王永闯 李立 王莉 俞春江 哈尔滨医科大学附属第二临床医院神经内科 哈尔滨医科大学附属第二临床医院老年病科 
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中文摘要:
      目的:在tau 过磷酸化大鼠中,通过检测淀粉样前体蛋白(amyloid precursor protein, APP)C末端片段的表达,研究抑制β- 分 泌酶(BACE1)对其代谢的影响及机制。方法:24 只SD大鼠随机分为四组,包括正常对照组、假手术组、OA 组、OA+BACE1 抑制剂 组。Western blot 法检测β-CTF、APP 及BACE1 表达;RT-PCR 法检测APP 及BACE1;水迷宫检测大鼠行为学。结果:OA 组 β-CTF表达显著增加(p<0.05),而OA+BACE1 抑制剂组与OA 组相比,β-CTF表达减少(p<0.05);四组大鼠的APP在蛋白及 mRNA 水平表达无显著差别(p>0.05);OA组BACE1 在蛋白及mRNA 水平的表达增加,而OA+BACE1 抑制剂组BACE1 的蛋 白表达较OA组减少(p<0.05),两组大鼠mRNA 表达水平无明显差异(p>0.05)。OA+BACE1 抑制剂组大鼠在给予BACE1 抑制剂 后行为学有所改善(p<0.05)。结论:⑴tau 过磷酸化通过促进神经元内BACE1 表达,导致APP代谢途径发生转变,从而引起茁-CTF 表达增加;⑵β-CTF表达增加可引起tau 过磷酸化大鼠行为学改变;⑶抑制BACE1 可改善大鼠的学习及记忆能力,支持BACE1 作为AD的治疗靶点。
英文摘要:
      Objective:To study the effects and mechanisms of β-secretase inhibitor on the processing of β-CTF in tau hyperphosphorylated rat model.Methods:Twenty-four male SD rats were randomly divided into four groups, including the control group, the sham group, the OA group and the OA+BACE1 group. For each group of rats, Western blot was used to analyze the level of amyloid precursor protein C-terminal fragment (APP-CTF), APP and BACE1. Meanwhile, RT-PCR was performed to detect the mRNA levels of APP and BACE1. With water maze test, abilities of learning and memory were detected.Results:It was found that β-CTF significantly increased in the OA group(p<0.05), while decreased in the OA + BACE1 inhibitor group compared to the OA group(p<0.05). There was no statistically significant difference in the protein and mRNA levels of APP among the four groups (p>0.05). The protein and mRNA levels of BACE1 significantly increased in the OA group (p<0.05). The protein levels of BACE1 in the OA+BACE1 inhibitor group decreased compared to the control group (p <0.05), and there was no difference in the mRNA levels between the two groups (p> 0.05). With water maze test, the behavior of rats in the OA+BACE1 inhibitor group were restored(p<0.05).Conclusion:⑴Hyperphosphorylated tau protein induced the increase of BACE1 expression, thus the pathway of APP processing had been shifted, and the level of β-CTF increased in neurons, ⑵The increase of β-CTF impaired the behavior of rats, ⑶ Inhibition of BACE1 could improve the abilities of study and memory in rats, indicating that BACE1 might be a therapeutic target of AD.
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