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Coenzyme Q_{10} and oxidative imbalance in Down syndrome: Biochemical and clinical aspects

机译:唐氏综合症中的辅酶Q_ {10}和氧化失衡:生化和临床方面

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摘要

Down syndrome (DS) is a chromosomal abnormality (trisomy 21) associated with mental retardation and Alzheimer-like dementia, characteristic change of the individual's phenotype and premature ageing. Oxidative stress is known to play a major role in this pathology since a gene dose effect leads to elevated ratio of superoxide dismutase to catalase/glutathione peroxidase compared to controls in all age categories suggesting that oxidative imbalance contributes to the clinical manifestation of DS. Hyperuricemia is another feature of DS that has an interesting relationship with oxidative stress since uric acid represents an important free radical scavenger. However its formation is connected to the conversion of Xanthine dehydrogenase (XDH) to Xanthine oxidase (XO) which leads to concomitant production of free radicals. Here we report that plasma samples from DS patients in pediatric age, despite an increased total antioxidant capacity, largely due to elevated Uric acid content (UA), present significantly elevated markers of oxidative damage such as increased allantoin levels. Moreover DS plasma samples do not differ from healthy control ones in terms of Coenzyme Q_{10} and susceptibility to peroxidative stimuli. On the contrary, lymphocyte and platelet CoQ_{10} content was significantly lower in DS patients, a fact that might underlie oxidative imbalance at a cellular level.
机译:唐氏综合症(DS)是一种染色体异常(21号三体症),与智力低下和阿尔茨海默氏样痴呆,个体表型的特征性变化以及过早衰老相关。众所周知,氧化应激在这种病理中起主要作用,因为与所有年龄段的对照相比,基因剂量效应导致超氧化物歧化酶与过氧化氢酶/谷胱甘肽过氧化物酶的比率升高,这表明氧化失衡有助于DS的临床表现。高尿酸血症是DS的另一个特征,它与氧化应激有着有趣的关系,因为尿酸是一种重要的自由基清除剂。然而,其形成与黄嘌呤脱氢酶(XDH)向黄嘌呤氧化酶(XO)的转化有关,这导致自由基的伴随产生。在这里我们报道,尽管总抗氧化剂能力增加(主要是由于尿酸含量(UA)升高),但小儿DS患者的血浆样品却呈现出明显的氧化损伤标记物,例如尿囊素水平升高。此外,DS血浆样品在辅酶Q_ {10}和对过氧化刺激的敏感性方面与健康对照组没有差异。相反,DS患者的淋巴细胞和血小板CoQ_ {10}含量明显较低,这一事实可能是细胞水平氧化不平衡的基础。

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  • 来源
    《BioFactors》 |2008年第4期|161-167|共7页
  • 作者单位

    Institute of Biochemistry, Polytechnic University of the Marche, Ancona, Italy;

    Pediatric Clinic Laboratory, Children Hospital Salesi, Polytechnic University of Marche, Ancona;

    Pediatric Clinic Laboratory, Children Hospital Salesi, Polytechnic University of Marche, Ancona;

    Pediatric Clinic Laboratory, Children Hospital Salesi, Polytechnic University of Marche, Ancona;

    Institute of Biochemistry, Polytechnic University of the Marche, Ancona, Italy;

    Institute of Biochemistry, Polytechnic University of the Marche, Ancona, Italy;

    Institute of Biochemistry, Polytechnic University of the Marche, Ancona, Italy;

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