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昼夜节律、氧化应激和抗氧化防御机制。

Circadian rhythms, oxidative stress, and antioxidative defense mechanisms.

作者信息

Hardeland Rüdiger, Coto-Montes Ana, Poeggeler Burkhard

机构信息

Institute of Zoology and Anthropology, University of Göttingen, Göttingen, Germany.

出版信息

Chronobiol Int. 2003 Nov;20(6):921-62. doi: 10.1081/cbi-120025245.

Abstract

Endogenous circadian and exogenously driven daily rhythms of antioxidative enzyme activities and of low molecular weight antioxidants (LMWAs) are described in various phylogenetically distant organisms. Substantial amplitudes are detected in several cases, suggesting the significance of rhythmicity in avoiding excessive oxidative stress. Mammalian and/or avian glutathione peroxidase and, as a consequence, glutathione reductase activities follow the rhythm of melatonin. Another hint for an involvement of melatonin in the control of redox processes is seen in its high-affinity binding to cytosolic quinone reductase 2, previously believed to be a melatonin receptor. Although antioxidative protection by pharmacological doses of melatonin is repeatedly reported, explanations of these findings are still insufficient and their physiological and chronobiological relevance is not yet settled. Recent data indicate a role of melatonin in the avoidance of mitochondrial radical formation, a function which may prevail over direct scavenging. Rhythmic changes in oxidative damage of protein and lipid molecules are also reported. Enhanced oxidative protein modification accompanied by a marked increase in the circadian amplitude of this parameter is detected in the Drosophila mutant rosy, which is deficient in the LMWA urate. Preliminary evidence for the significance of circadian rhythmicity in diminishing oxidative stress comes from clock mutants. In Drosophila, moderately enhanced protein damage is described for the arrhythmic and melatonin null mutant per0, but even more elevated, periodic damage is found in the short-period mutant per(s), synchronized to LD 12:12. Remarkably large increases in oxidative protein damage, along with impairment of tissue integrity and--obviously insufficient--compensatory elevations in protective enzymes are observed in a particularly vulnerable organ, the Harderian gland, of another short-period mutant tau, in the Syrian hamster. Mice deficient in the per2 gene homolog are reported to be cancer-prone, a finding which might also relate to oxidative stress. In the dinoflagellate Lingulodinium polyedrum [Gonyaulax polyedra], various treatments that cause oxidative stress result in strong suppressions of melatonin and its metabolite 5-methoxytryptamine (5-MT) and to secondary effects on overt rhythmicity. The glow maximum, depending on the presence of elevated 5-MT at the end of subjective night, decreases in a dose-dependent manner already under moderate, non-lethal oxidative stress, but is restored by replenishing melatonin. Therefore, a general effect of oxidative stress may consist in declines of easily oxidizable signaling molecules such as melatonin, and this can have consequences on the circadian intraorganismal organization and expression of overt rhythms. Recent findings on a redox-sensitive input into the core oscillator via modulation of NPAS2/BMAL1 or CLK/BMAL1 heterodimer binding to DNA indicate a direct influence of cellular redox balance, including oxidative stress, on the circadian clock.

摘要

在各种系统发育关系较远的生物体中,均描述了抗氧化酶活性以及低分子量抗氧化剂(LMWAs)的内源性昼夜节律和外源性驱动的每日节律。在一些情况下检测到了较大的振幅,这表明节律性对于避免过度氧化应激具有重要意义。哺乳动物和/或鸟类的谷胱甘肽过氧化物酶以及由此产生的谷胱甘肽还原酶活性遵循褪黑素的节律。褪黑素与胞质醌还原酶2具有高亲和力结合,这一现象暗示了褪黑素参与氧化还原过程的调控,胞质醌还原酶2此前被认为是一种褪黑素受体。尽管多次报道了药理剂量的褪黑素具有抗氧化保护作用,但对这些发现的解释仍然不足,其生理和生物钟学相关性尚未确定。最近的数据表明,褪黑素在避免线粒体自由基形成中发挥作用,这一功能可能比直接清除自由基更为重要。也有报道称蛋白质和脂质分子的氧化损伤存在节律性变化。在果蝇突变体rosy中检测到氧化蛋白质修饰增强,同时该参数的昼夜振幅显著增加,rosy突变体缺乏LMWAs尿酸盐。生物钟突变体的研究初步证明了昼夜节律性在减轻氧化应激方面的重要性。在果蝇中,无节律和褪黑素缺失突变体per0的蛋白质损伤有适度增强,但在与LD 12:12同步的短周期突变体per(s)中发现了更明显的周期性损伤。在叙利亚仓鼠的另一个短周期突变体tau的特别脆弱的器官——哈德氏腺中,观察到氧化蛋白质损伤显著增加,同时组织完整性受损,保护酶的补偿性升高明显不足。据报道,per2基因同源物缺陷的小鼠易患癌症,这一发现也可能与氧化应激有关。在甲藻多甲藻[多甲藻]中,各种导致氧化应激的处理会导致褪黑素及其代谢物5-甲氧基色胺(5-MT)受到强烈抑制,并对明显的节律性产生次生影响。取决于主观夜间结束时5-MT的升高情况,发光最大值在中度、非致死性氧化应激下就已经以剂量依赖的方式降低,但补充褪黑素后可恢复。因此,氧化应激的一般影响可能包括易氧化信号分子如褪黑素的减少,这可能会对生物钟在体内的组织和明显节律的表达产生影响。最近关于通过调节NPAS2/BMAL1或CLK/BMAL1异二聚体与DNA的结合对核心振荡器进行氧化还原敏感输入的研究结果表明,细胞氧化还原平衡,包括氧化应激,对生物钟有直接影响。

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