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首页> 外文期刊>Brain pathology >Metaflammasome components in the human brain: a role in dementia with Alzheimer's pathology?
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Metaflammasome components in the human brain: a role in dementia with Alzheimer's pathology?

机译:人体大脑中的metaFlammasome组件:痴呆症与阿尔茨海默氏病病的作用?

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摘要

Epidemiological and genetic studies have identified metabolic disorders and inflammation as risk factors for Alzheimer's disease (AD). Evidence in obesity and type-2 diabetes suggests a role for a metabolic inflammasome (metaflammasome) in mediating chronic inflammation in peripheral organs implicating IKK (inhibitor of nuclear factor kappa-B kinase subunit beta), IRS1 (insulin receptor substrate 1), JNK (c-jun N-terminal kinase), and PKR (double-stranded RNA protein kinase). We hypothesized that these proteins are expressed in the brain in response to metabolic risk factors in AD. Neocortex from 299 participants from the MRC Cognitive Function and Ageing Studies was analysed by immunohistochemistry for the expression of the phosphorylated (active) form of IKK [pSer(176/180)], IRS1 [pS(312)], JNK [pThr(183)/Tyr(185)] and PKR [pT(451)]. The data were analyzed to investigate whether the proteins were expressed together and in relation with metabolic disorders, dementia, Alzheimer's pathology and APOE genotype. We observed a change from a positive to a negative association between the proteins and hypertension according to the dementia status. Type-2 diabetes was negatively related with the proteins among participants without dementia; whereas participants with dementia and AD pathology showed a positive association with JNK. A significant association between IKK and JNK in participants with dementia and AD pathology was observed, but not in those without dementia. Otherwise, weak to moderate associations were observed among the protein loads. The presence of dementia was significantly associated with JNK and negatively associated with IKK and IRS1. Cognitive scores showed a significant positive relationship with IKK and a negative with IRS1, JNK and PKR. The proteins were significantly associated with pathology in Alzheimer's participants with the relationship being inverse or not significant in participants without dementia. Expression of the proteins was not related to APOE genotype. These findings highlight a role for these proteins in AD pathophysiology but not necessarily as a complex.
机译:流行病学和遗传学研究已经确定了代谢障碍和阿尔茨海默病(AD)的危险因素。肥胖症和2型糖尿病的证据表明,代谢涌入(Metaflammasome)在暗示IKK(核因子Kappa-B激酶亚基酶β),IRS1(胰岛素受体基质1),JNK( C-JUM N-末端激酶)和PKR(双链RNA蛋白激酶)。我们假设这些蛋白质在大脑中表达,以应对广告中的代谢危险因素。从MRC认知功能和老化研究中的299名参与者的Neocortex进行了免疫组织化学,用于表达磷酸化(活性)形式的IKK [PSER(176/180)],IRS1 [PS(312)],JNK [PTHR(183 )/ tyr(185)]和pkr [pt(451)]。分析数据以研究蛋白质是否在一起表达,并与代谢紊乱,痴呆,阿尔茨海默病病理和ApoE基因型相关。根据痴呆状态,我们观察到蛋白质和高血压之间的阳性至负关联的变化。 2型糖尿病与参与者之间的蛋白质与没有痴呆的蛋白质负相关;虽然参与者和痴呆症和广告病理学表现出与JNK的积极关系。观察到痴呆症和AD病理学的参与者中IKK和JNK之间的重要关联,但不在那些没有痴呆的人中。否则,在蛋白质载荷之间观察到弱到中度关联。痴呆的存在与JNK显着相关,与IKK和IRS1负相关。认知评分与IKK和IRS1,JNK和PKR的负面的阳性关系显示出显着的正相关关系。在没有痴呆的参与者中,蛋白质与阿尔茨海默氏症的参与者的病理学显着相关。蛋白质的表达与ApoE基因型无关。这些发现突出了广告病理学中这些蛋白质的作用,但不一定是复杂的。

著录项

  • 来源
    《Brain pathology》 |2017年第3期|共10页
  • 作者单位

    Univ Southampton Clin Neurosci Clin &

    Expt Sci Acad Unit Fac Med Southampton Hants England;

    Univ Cambridge Inst Publ Hlth Dept Publ Hlth &

    Primary Care Cambridge England;

    Univ Southampton Clin Neurosci Clin &

    Expt Sci Acad Unit Fac Med Southampton Hants England;

    Cambridge Inst Publ Hlth MRC Biostat Unit Cambridge England;

    Univ Cambridge Inst Publ Hlth Dept Publ Hlth &

    Primary Care Cambridge England;

    Univ Sheffield Sheffield Inst Translat Neurosci Dept Neurosci Sheffield S Yorkshire England;

    Univ Southampton Clin Neurosci Clin &

    Expt Sci Acad Unit Fac Med Southampton Hants England;

    INSERM U942 Paris France;

    Univ Southampton Clin Neurosci Clin &

    Expt Sci Acad Unit Fac Med Southampton Hants England;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 病理学;
  • 关键词

    dementia; metaflammasome; CFAS; Alzheimer's disease; human brain;

    机译:痴呆症;metaflammasome;cfas;阿尔茨海默病;人脑;

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