Miyazaki Ikuko, Asanuma Masato, Hozumi Hiroaki, Miyoshi Ko, Sogawa Norio
Department of Brain Science, Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, 2-5-1 Shikatacho, Okayama 700-8558, Japan.
FEBS Lett. 2007 Oct 16;581(25):5003-8. doi: 10.1016/j.febslet.2007.09.046. Epub 2007 Sep 29.
Dopamine (DA) quinone as DA neuron-specific oxidative stress conjugates with cysteine residues in functional proteins to form quinoproteins. Here, we examined the effects of cysteine-rich metal-binding proteins, metallothionein (MT)-1 and -2, on DA quinone-induced neurotoxicity. MT quenched DA semiquinones in vitro. In dopaminergic cells, DA exposure increased quinoproteins and decreased cell viability; these were ameliorated by pretreatment with MT-inducer zinc. Repeated L-DOPA administration markedly elevated striatal quinoprotein levels and reduced the DA nerve terminals specifically on the lesioned side in MT-knockout parkinsonian mice, but not in wild-type mice. Our results suggested that intrinsic MT protects against L-DOPA-induced DA quinone neurotoxicity in parkinsonian mice by its quinone-quenching property.
多巴胺(DA)醌作为DA神经元特异性氧化应激产物,与功能蛋白中的半胱氨酸残基结合形成醌蛋白。在此,我们研究了富含半胱氨酸的金属结合蛋白金属硫蛋白(MT)-1和-2对DA醌诱导的神经毒性的影响。MT在体外淬灭DA半醌。在多巴胺能细胞中,暴露于DA会增加醌蛋白并降低细胞活力;MT诱导剂锌预处理可改善这些情况。在MT基因敲除的帕金森病小鼠中,反复给予左旋多巴可显著提高纹状体醌蛋白水平,并特异性降低损伤侧的DA神经末梢,但在野生型小鼠中则不会。我们的结果表明,内源性MT通过其醌淬灭特性保护帕金森病小鼠免受左旋多巴诱导的DA醌神经毒性。
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