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Effects and possible mechanisms of action of acacetin on the behavior and eye morphology of Drosophila models of Alzheimer’s disease

机译:阿卡西汀对阿尔茨海默病果蝇模型的行为和眼部形态的影响及其可能的作用机制

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The human β-amyloid (Aβ) cleaving enzyme (BACE-1) is a target for Alzheimer’s disease (AD) treatments. This study was conducted to determine if acacetin extracted from the whole Agastache rugosa plant had anti-BACE-1 and behavioral activities in Drosophila melanogaster AD models and to determine acacetin’s mechanism of action. Acacetin (100, 300, and 500?μM) rescued amyloid precursor protein (APP)/BACE1-expressing flies and kept them from developing both eye morphology (dark deposits, ommatidial collapse and fusion, and the absence of ommatidial bristles) and behavioral (motor abnormalities) defects. The reverse transcription polymerase chain reaction analysis revealed that acacetin reduced both the human APP and BACE-1 mRNA levels in the transgenic flies, suggesting that it plays an important role in the transcriptional regulation of human BACE-1 and APP . Western blot analysis revealed that acacetin reduced Aβ production by interfering with BACE-1 activity and APP synthesis, resulting in a decrease in the levels of the APP carboxy-terminal fragments and the APP intracellular domain. Therefore, the protective effect of acacetin on Aβ production is mediated by transcriptional regulation of BACE-1 and APP , resulting in decreased APP protein expression and BACE-1 activity. Acacetin also inhibited APP synthesis, resulting in a decrease in the number of amyloid plaques.
机译:人β淀粉样蛋白(Aβ)裂解酶(BACE-1)是阿尔茨海默氏病(AD)治疗的目标。进行这项研究的目的是确定从整株皱叶ast香植物中提取的阿卡西汀在果蝇AD模型中是否具有抗BACE-1和行为活性,并确定阿卡西汀的作用机理。 Acacetin(100、300和500?μM)挽救了表达淀粉样前体蛋白(APP)/ BACE1的果蝇,并阻止了它们形成眼睛的形态(暗沉,虫眼塌陷和融合,并且没有虫眼硬毛)和行为(运动异常)缺陷。逆转录聚合酶链反应分析表明,醋氨蝶呤降低了转基因果蝇中人APP和BACE-1 mRNA的水平,表明它在人BACE-1和APP的转录调控中起重要作用。蛋白质印迹分析表明,醋氨蝶呤通过干扰BACE-1活性和APP合成来减少Aβ的产生,从而导致APP羧基末端片段和APP细胞内结构域水平的降低。因此,Acacetin对Aβ产生的保护作用是由BACE-1和APP的转录调控介导的,导致APP蛋白表达和BACE-1活性降低。 Acacetin还抑制APP合成,导致淀粉样斑块数量减少。

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