氧化应激
材料科学
活性氧
纳米医学
神经退行性变
纳米颗粒
抗氧化剂
化学
医学
生物物理学
生物化学
纳米技术
生物
疾病
内科学
作者
Lei Zhang,Penghe Zhao,Caiping Yue,Zhaokui Jin,Qiong Liu,Xiubo Du,Qianjun He
出处
期刊:Biomaterials
[Elsevier]
日期:2019-01-25
卷期号:197: 393-404
被引量:120
标识
DOI:10.1016/j.biomaterials.2019.01.037
摘要
Oxidative stress-induced mitochondrial dysfunction plays an important role in the pathogenesis of Alzheimer's disease (AD). Hydrogen molecule, a special antioxidant, can selectively scavenge highly cytotoxic reactive oxygen species such as ·OH, exhibiting a potential to treat AD by reducing oxidative stress. However, there is no effective route to realize the continuous and efficient accumulation of administrated hydrogen in AD brain owing to its low solubility. Here, we develop the small-sized Pd hydride (PdH) nanoparticles for high payload of hydrogen and in situ sustained hydrogen release in AD brain. By virtue of the catalytic hydrogenation effect of Pd, the released hydrogen from PdH nanoparticles exhibits high bio-reductivity in favor of effectively scavenging cytotoxic ·OH in a self-catalysis way. Bio-reductive hydrogen is able to recover mitochondrial dysfunction, inhibit Aβ generation and aggregation, block synaptic and neuronal apoptosis and promote neuronal energy metabolism by eliminating oxidative stress and activating the anti-oxidative pathway, consequently ameliorating the cognitive impairment in AD mice. The proposed hydrogen-releasing nanomedicine strategy would open a new window for the treatment of AD.
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