Saeed Kamran, Shah Shahid Ali, Ullah Rahat, Alam Sayed Ibrar, Park Jun Sung, Saleem Samreen, Jo Myeung Hoon, Kim Min Woo, Hahm Jong Ryeal, Kim Myeong Ok
Division of Life Sciences and Applied Life Science (BK 21plus), College of Natural Science, Gyeongsang National University, Jinju 52828, Republic of Korea.
Faculty of Allied Health Sciences and Technologies, Women University Swabi, Pakistan.
Oxid Med Cell Longev. 2020 Nov 20;2020:9523758. doi: 10.1155/2020/9523758. eCollection 2020.
Alzheimer's disease (AD) is a progressive neurodegenerative disorder typified by several neuropathological features including amyloid-beta (A) plaque and neurofibrillary tangles (NFTs). Cholesterol retention and oxidative stress (OS) are the major contributors of elevated - and -secretase activities, leading to excessive A deposition, signifying the importance of altered cholesterol homeostasis and OS in the progression of A-mediated neurodegeneration and cognitive deficit. However, the effect of A on cholesterol metabolism is lesser-known. In this study, we evaluated the effect of quinovic acid (QA; 50 mg/kg body weight, i.p.) against the intracerebroventricular (i.c.v.) injection of A (1-42)-induced cholesterol dyshomeostasis, oxidative stress, and neurodegeneration in the cortex and hippocampal brain regions of wild-type male C57BL/6J mice. Our results indicated that A (1-42)-treated mice have increased A oligomer formation along with increased -secretase expression. The enhanced amyloidogenic pathway in A (1-42)-treated mice intensified brain cholesterol accumulation due to increased expressions of p53 and 3-hydroxy-3-methylglutaryl-CoA reductase (HMGCR) enzyme. Importantly, we further confirmed the p53-mediated HMGCR axis activation by using pifithrin- (PFT) in SH-SY5Y cells. Furthermore, the augmented brain cholesterol levels were also associated with increased OS. However, the QA administration to A (1-42)-injected mice significantly ameliorated the A burden, p53 expression, and cholesterol accumulation by deterring the oxidative stress through upregulating the Nrf2/HO-1 pathway. Moreover, the QA downregulated gliosis, neuroinflammatory mediators (p-NF-B and IL-1), and the expression of mitochondrial apoptotic markers (Bax, cleaved caspase-3, and cytochrome c). QA treatment also reversed the deregulated synaptic markers (PSD-95 and synaptophysin) and improved spatial learning and memory behaviors in the A-treated mouse brains. These results suggest that A (1-42) induces its acute detrimental effects on cognitive functions probably by increasing brain cholesterol levels through a possible activation of the p53/HMGCR axis. However, QA treatment reduces the cholesterol-induced oxidative stress, neuroinflammation, and neurodegeneration, leading to the restoration of cognitive deficit after A (1-42) i.c.v. injection in mice.
阿尔茨海默病(AD)是一种进行性神经退行性疾病,其特征为多种神经病理学特征,包括β淀粉样蛋白(Aβ)斑块和神经原纤维缠结(NFTs)。胆固醇潴留和氧化应激(OS)是导致β-和γ-分泌酶活性升高的主要因素,进而导致Aβ过度沉积,这表明胆固醇稳态改变和OS在Aβ介导的神经退行性变和认知缺陷进展中具有重要意义。然而,Aβ对胆固醇代谢的影响鲜为人知。在本研究中,我们评估了奎诺酸(QA;50mg/kg体重,腹腔注射)对野生型雄性C57BL/6J小鼠脑室内(i.c.v.)注射Aβ(1-42)诱导的胆固醇稳态失调、氧化应激以及皮质和海马脑区神经退行性变的影响。我们的结果表明,用Aβ(1-42)处理的小鼠Aβ寡聚体形成增加,同时γ-分泌酶表达增加。在Aβ(1-42)处理的小鼠中,增强的淀粉样蛋白生成途径由于p53和3-羟基-3-甲基戊二酰辅酶A还原酶(HMGCR)酶表达增加而加剧了脑胆固醇积累。重要的是,我们在SH-SY5Y细胞中使用pifithrin-α(PFT)进一步证实了p53介导的HMGCR轴激活。此外,脑胆固醇水平升高还与OS增加有关。然而,对注射Aβ(1-42)的小鼠给予QA可通过上调Nrf2/HO-1途径减轻氧化应激,从而显著改善Aβ负担、p53表达和胆固醇积累。此外,QA下调了胶质增生、神经炎症介质(p-NF-κB和IL-1)以及线粒体凋亡标志物(Bax、裂解的caspase-3和细胞色素c)的表达。QA治疗还逆转了失调的突触标志物(PSD-95和突触素),并改善了Aβ处理的小鼠脑内的空间学习和记忆行为。这些结果表明,Aβ(1-42)可能通过激活p53/HMGCR轴增加脑胆固醇水平,从而对认知功能产生急性有害影响。然而,QA治疗可降低胆固醇诱导的氧化应激、神经炎症和神经退行性变,导致小鼠脑室内注射Aβ(1-42)后认知缺陷得到恢复。
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