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Mechanisms of immunosenescence: lessons from models of accelerated immune aging

机译:免疫衰老的机制:加速免疫衰老模型的教训

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摘要

With increasing age, the ability of the adaptive immune system to respond to vaccines and to protect from infection declines. In parallel, the production of inflammatory mediators increases. While cross-sectional studies have been successful in denning age-dependent immunological phenotypes, studies of accelerated immune aging in human subpopulations have been instrumental in obtaining mechanistic insights. The immune system depends on its regen erative capacity; however, the T cell repertoire, once established, is relatively robust to aging and only decompensates when additionally stressed. Such stressors include chronic infections such as CMV and HIV, even when viral repli cation is controlled, and autoimmune diseases. Reduced regenerative capacity, chronic immune activation in the absence of cell exhaustion, T cell memory inflation, and accumulation of highly potent effector T cells in these patients synergize to develop an immune phenotype that is characteristic of the elderly. Studies of accelerated immune aging in autoimmune diseases have identified an unexpected link to chronic DNA damage responses that are known to be important in aging, but so far had not been implicated in immune aging.
机译:随着年龄的增长,适应性免疫系统对疫苗作出反应并防止感染的能力下降。同时,炎症介质的产生增加。尽管横断面研究已成功地确定了年龄依赖性免疫表型,但研究人类亚群中加速免疫老化的研究已在获得机械学见解方面发挥了重要作用。免疫系统取决于其再生能力。然而,一旦建立了T细胞库,它对衰老就相对健壮,并且仅在受到额外压力时才会失代偿。即使在病毒复制受到控制的情况下,此类应激源也包括慢性感染,例如CMV和HIV,以及自身免疫性疾病。在这些患者中,再生能力降低,在没有细胞衰竭的情况下进行慢性免疫激活,T细胞记忆膨胀以及在这些患者中高效率的效应T细胞蓄积可协同发展出老年人特有的免疫表型。在自身免疫性疾病中加速免疫衰老的研究已经确定了与慢性DNA损伤反应的出乎意料的联系,众所周知,慢性DNA损伤反应对衰老很重要,但到目前为止,尚未涉及免疫衰老。

著录项

  • 来源
    《Annals of the New York Academy of Sciences》 |2012年第2012期|p.69-82|共14页
  • 作者单位

    Department of Medicine, Division of Immunology and Rheumatology, Stanford University School of Medicine, Stanford,California and Palo Alto Department of Veterans Affairs Health Care System, Palo Alto, California;

    Department of Medicine, Division of Immunology and Rheumatology, Stanford University School of Medicine, Stanford,California and Palo Alto Department of Veterans Affairs Health Care System, Palo Alto, California;

    Department of Medicine, Division of Immunology and Rheumatology,Stanford University School of Medicine CCSR Building, Room 2215, Mail Code 5166 269 Campus Drive West Stanford, CA 94305-5166;

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  • 原文格式 PDF
  • 正文语种 eng
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  • 关键词

    immune aging; thymic involution; HIV; CMV; autoimmunity; latency;

    机译:免疫衰老胸腺退化艾滋病病毒;CMV;自身免疫潜伏;

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