Yang Ying, Chen Wei, Wang Xiaoming, Ge Wei
Department of General Practice, Xijing Hospital, Fourth Military Medical University, Xi'an 710032, China.
Department of Geriatrics, Xijing Hospital, Fourth Military Medical University, Xi'an 710032, China.
Acta Biochim Biophys Sin (Shanghai). 2021 Jul 5;53(7):837-847. doi: 10.1093/abbs/gmab057.
Alzheimer's disease (AD) is one of the major life-threatening diseases for the elderly because neither pathogenesis nor effective treatment is available. Mitochondrial aldehyde dehydrogenase 2 (ALDH2) has been shown to reduce the cell-damaging aldehydes in response to reactive oxygen species (ROS). However, whether it plays a role in AD remains elusive. In the present study, we found that ALDH2 overexpression significantly improved the cognitive function of the AD mouse. Behavioral analyses of ALDH2-overexpressing APP/PS1 AD mice showed that the learning and cognitive abilities were significantly higher in these mice than in the control group APP/PS1 mice. Further open-field behavior experiments showed the same results. At the cellular level, ALDH2 protects nerve cells. HT22 cells were challenged with Aβ to establish an AD cell model, in the presence or absence of the ALDH2 activator Alda-1 and ALDH2 inhibitor Daidzin. Incubation with 50 μM Aβ for 24 h significantly reduced HT22 cell survival and cell viability, the effects of which were attenuated by the ALDH2 activator Alda-1 (50 μM). Aβ challenge promoted apoptosis and upregulated caspase3 level but suppressed Bcl-2 level, and the upregulated caspase3 level was reversed by the ALDH-2 agonist Alda-1. Aβ-induced clonal ball abnormal was reversed by Alda-1. Aβ altered the mitochondria geometry evidenced by vacuolar degeneration and membrane rupture, whereas Alda-1 changed the Aβ-induced mitochondria geometry anomalies. Moreover, superoxide anion and toxic 4-hydroxy-nonanal (4-HNE) and ROS increased by Aβ challenge were reversed by Alda-1. Meanwhile, Aβ-induced ATP reduction was reversed by Alda-1. Taken together, ALDH2 overexpression significantly improves the cognitive function of the AD mice. Furthermore, our results suggested that ALDH2 protects against Aβ hippocampal neuronal toxicity possibly through alleviating toxic aldehydes and ROS, as well as increasing ATP production to preserve mitochondrial integrity and reduce neuronal apoptosis.
阿尔茨海默病(AD)是老年人面临的主要危及生命的疾病之一,因为其发病机制不明且尚无有效治疗方法。线粒体乙醛脱氢酶2(ALDH2)已被证明可响应活性氧(ROS)减少细胞损伤性醛类物质。然而,其在AD中是否发挥作用仍不清楚。在本研究中,我们发现ALDH2过表达显著改善了AD小鼠的认知功能。对过表达ALDH2的APP/PS1 AD小鼠进行行为分析表明,这些小鼠的学习和认知能力显著高于对照组APP/PS1小鼠。进一步的旷场行为实验也得到了相同结果。在细胞水平上,ALDH2可保护神经细胞。在存在或不存在ALDH2激活剂Alda-1和ALDH2抑制剂大豆苷的情况下,用Aβ刺激HT22细胞以建立AD细胞模型。用50μM Aβ孵育24小时显著降低了HT22细胞的存活率和细胞活力,而ALDH2激活剂Alda-1(50μM)可减弱这些影响。Aβ刺激促进了细胞凋亡并上调了caspase3水平,但抑制了Bcl-2水平,而ALDH-2激动剂Alda-1可逆转上调的caspase3水平。Alda-1可逆转Aβ诱导的克隆球异常。Aβ改变了线粒体形态,表现为空泡变性和膜破裂,而Alda-1改变了Aβ诱导的线粒体形态异常。此外,Aβ刺激增加的超氧阴离子、有毒的4-羟基壬烯醛(4-HNE)和ROS被Alda-1逆转。同时,Aβ诱导的ATP减少也被Alda-1逆转。综上所述,ALDH2过表达显著改善了AD小鼠的认知功能。此外,我们的结果表明,ALDH2可能通过减轻有毒醛类物质和ROS,以及增加ATP生成以维持线粒体完整性和减少神经元凋亡来保护海马神经元免受Aβ毒性。
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