Size- and Age-Dependent Neurotoxicity of Engineered Metal Nanoparticles in Rats

被引:0
|
作者
Aruna Sharma
Dafin F. Muresanu
Ranjana Patnaik
Hari S. Sharma
机构
[1] Uppsala University Hospital,Laboratory of Cerebrovascular Research, Department of Surgical Sciences, Anesthesiology and Intensive Care Medicine
[2] University of Medicine and Pharmacy,Department of Neurosciences, University Hospital
[3] Banaras Hindu University,Department of Biomaterials, School of Biomedical Engineering, National Institute of Technology
来源
Molecular Neurobiology | 2013年 / 48卷
关键词
Metal nanoparticles; Size; Age; Neurotoxicity; Blood–brain barrier; Brain edema; Neuronal injuries; Nitric oxide; Neuropathology;
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摘要
Earlier we showed that chronic administration of engineered nanoparticles (NPs) from metals, e.g., Cu, Ag, or Al (50–60 nm, 50 mg/kg, i.p. daily for 1 week) alter blood–brain barrier (BBB) disruption and induce brain pathology in adult rats (age 18 to 22 weeks). However, effects of size-dependent neurotoxicity of NPs in vivo are still largely unknown. In present investigation, we examined the effects of different size ranges of the above-engineered NPs on brain pathology in rats. Furthermore, the fact that age is also an important factor in brain pathology was also investigated in our rat model. Our results showed that small-sized NPs induced the most pronounced BBB breakdown (EBA +480 to 680 %; radioiodine +850 to 1025 %), brain edema formation (+4 to 6 %) and neuronal injuries (+30 to 40 %), glial fibrillary acidic protein upregulation (+40 to 56 % increase), and myelin vesiculation (+30 to 35 % damage) in young animals as compared to controls. Interestingly, the oldest animals (30 to 35 weeks of age) also showed massive brain pathology as compared to young adults (18 to 20 weeks old). The Ag and Cu exhibited greater brain damage compared with Al NPs in all age groups regardless of their size. This suggests that apart from the size, the composition of NPs is also important in neurotoxicity. The very young and elderly age groups exhibited greater neurotoxicity to NPs suggests that children and elderly are more vulnerable to NPs-induced brain damage. The NPs-induced brain damage correlated well with the upregulation of neuronal nitric oxide synthase activity in the brain indicating that NPs-induced neurotoxicity may be mediated via increased production of nitric oxide, not reported earlier.
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页码:386 / 396
页数:10
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