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首页> 外文期刊>Metallomics >Zinc, copper, and carnosine attenuate neurotoxicity of prion fragment PrP106-126
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Zinc, copper, and carnosine attenuate neurotoxicity of prion fragment PrP106-126

机译:锌,铜和肌氨酸减弱of病毒片段PrP106-126的神经毒性

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摘要

Prion diseases are progressive neurodegenerative diseases that are associated with the conversion of normal cellular prion protein (PrPC) to abnormal pathogenic prion protein (PrPSC) by conformational changes. Prion protein is a metal-binding protein that is suggested to be involved in metal homeostasis. We investigated here the effects of trace elements on the conformational changes and neurotoxicity of synthetic prion peptide (PrP106-126). PrP106-126 exhibited the formation of β-sheet structures and enhanced neurotoxicity during the aging process. The co-existence of Zn2+ or Cu2+ during aging inhibited β-sheet formation by PrP106-126 and attenuated its neurotoxicity on primary cultured rat hippocampal neurons. Although PrP106-126 formed amyloid-like fibrils as observed by atomic force microscopy, the height of the fibers was decreased in the presence of Zn2+ or Cu2+. Carnosine (β-alanyl histidine) significantly inhibited both the β-sheet formation and the neurotoxicity of PrP106-126. Our results suggested that Zn2+ and Cu2+ might be involved in the pathogenesis of prion diseases. It is also possible that carnosine might become a candidate for therapeutic treatments for prion diseases.
机译:on病毒疾病是进行性神经退行性疾病,与正常细胞cellular蛋白(PrP C )通过构象变化转化为致病性pr病毒蛋白(PrP SC )有关。 on病毒蛋白是一种金属结合蛋白,被认为与金属稳态有关。我们在这里研究了微量元素对合成病毒肽(PrP106-126)的构象变化和神经毒性的影响。 PrP106-126在衰老过程中表现出β-折叠结构的形成并增强了神经毒性。衰老过程中Zn 2 + 或Cu 2 + 的共存抑制了PrP106-126形成的β-折叠,并减弱了其对原代培养的大鼠海马神经元的神经毒性。尽管通过原子力显微镜观察到PrP106-126形成淀粉样样原纤维,但是在Zn 2 + 或Cu 2 + 存在的情况下纤维的高度却降低了。肌肽(β-丙氨酰组氨酸)显着抑制PrP106-126的β-折叠形成和神经毒性。我们的研究结果提示Zn 2 + 和Cu 2 + 可能与pr病毒的发病有关。肌肽也可能成为病毒疾病治疗方法的候选者。

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  • 来源
    《Metallomics》 |2011年第7期|p.726-734|共9页
  • 作者单位

    1. Department of Analytical Chemistry,School of Pharmaceutical Sciences Kyushu University of Health and Welfare, 1714-1 Yoshino-cho, Nobeoka-shi, Miyazaki 882-8508, Japan;

    1. Department of Analytical Chemistry,School of Pharmaceutical Sciences Kyushu University of Health and Welfare, 1714-1 Yoshino-cho, Nobeoka-shi, Miyazaki 882-8508, Japan;

    1. Department of Analytical Chemistry,School of Pharmaceutical Sciences Kyushu University of Health and Welfare, 1714-1 Yoshino-cho, Nobeoka-shi, Miyazaki 882-8508, Japan;

    1. Department of Analytical Chemistry,School of Pharmaceutical Sciences Kyushu University of Health and Welfare, 1714-1 Yoshino-cho, Nobeoka-shi, Miyazaki 882-8508, Japan;

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