Immunosenescence in aging: between immune cells depletion and cytokines up-regulation.

Q2 Medicine

Clinical and Molecular Allergy Pub Date : 2017-12-14 eCollection Date: 2017-01-01 DOI:10.1186/s12948-017-0077-0

Maria Teresa Ventura, Marco Casciaro, Sebastiano Gangemi, Rosalba Buquicchio

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引用次数: 243

Abstract

Background: The immunosenescence is a relatively recent chapter, correlated with the linear extension of the average life began in the nineteenth century and still in progress. The most important feature of immunosenescence is the accumulation in the "immunological space" of memory and effector cells as a result of the stimulation caused by repeated clinical and subclinical infections and by continuous exposure to antigens (inhalant allergens, food, etc.). This state of chronic inflammation that characterizes senescence has a significant impact on survival and fragility. In fact, the condition of frail elderly occurs less frequently in situations characterized by poor contact with viral infections and parasitic diseases. Furthermore the immunosenescence is characterized by a particular "remodelling" of the immune system, induced by oxidative stress. Apoptosis plays a central role in old age, a period in which the ability of apoptosis can change. The remodelling of apoptosis, together with the Inflammaging and the up-regulation of the immune response with the consequent secretion of pro-inflammatory lymphokines represents the major determinant of the rate of aging and longevity, as well as of the most common diseases related with age and with tumors. Other changes occur in the innate immunity, the first line of defence providing rapid, but unspecific and incomplete protection, consisting mostly of monocytes, natural killer cells and dendritic cells, acting up to the establishment of a adaptive immune response, which is slower, but highly specific, which cellular substrate consists of T and B lymphocytes. The markers of "Inflammaging" in adaptive immunity in centenarians are characterized by a decrease in T cells "naive." The reduction of CD8 virgins may be related to the risk of morbidity and death, as well as the combination of the increase of CD8+ cells and reduction of CD4+ T cells and the reduction of CD19+ B cells. The immune function of the elderly is weakened to due to the exhaustion of T cell-virgin (CD95-), which are replaced with the clonal expansion of CD28-T cells.

Conclusions: The increase of pro-inflammatory cytokines is associated with dementia, Parkinson's disease, atherosclerosis, diabetes type 2, sarcopenia and a high risk of morbidity and mortality. A correct modulation of immune responses and apoptotic phenomena can be useful to reduce age-related degenerative diseases, as well as inflammatory and neoplastic diseases.

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衰老中的免疫衰老:免疫细胞耗竭与细胞因子上调之间的关系。

背景:免疫衰老是一个相对较新的篇章，与平均寿命的线性延长有关，始于19世纪，至今仍在进行中。免疫衰老最重要的特征是，由于反复的临床和亚临床感染以及持续暴露于抗原(吸入性过敏原、食物等)所引起的刺激，记忆细胞和效应细胞在“免疫空间”中积累。这种以衰老为特征的慢性炎症状态对生存和脆弱性有重大影响。事实上，在与病毒感染和寄生虫病接触较少的情况下，年老体弱的情况发生的频率较低。此外，免疫衰老的特征是氧化应激诱导的免疫系统的特殊“重塑”。细胞凋亡在老年中起着中心作用，这是细胞凋亡能力发生变化的时期。细胞凋亡的重塑，以及免疫反应的炎症和上调，以及随之而来的促炎淋巴因子的分泌，是衰老和长寿速度的主要决定因素，也是与年龄和肿瘤相关的最常见疾病的主要决定因素。其他变化发生在先天免疫中，这是提供快速但非特异性和不完全保护的第一道防线，主要由单核细胞、自然杀伤细胞和树突状细胞组成，起到建立适应性免疫反应的作用，这种反应较慢，但高度特异性，其细胞底物由T淋巴细胞和B淋巴细胞组成。百岁老人适应性免疫中的“炎症”标记以“幼稚”T细胞减少为特征。CD8处女的减少可能与发病和死亡的风险有关，也可能与CD8+细胞增加和CD4+ T细胞减少以及CD19+ B细胞减少的结合有关。由于T细胞处女(CD95-)的耗尽，老年人的免疫功能减弱，取而代之的是CD28-T细胞的克隆扩增。结论:促炎细胞因子的升高与痴呆、帕金森病、动脉粥样硬化、2型糖尿病、肌肉减少症以及高发病率和死亡率相关。正确调节免疫反应和细胞凋亡现象有助于减少与年龄相关的退行性疾病，以及炎症和肿瘤疾病。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical and Molecular Allergy Medicine-Immunology and Allergy

CiteScore

8.20

自引率

0.00%

发文量

审稿时长

13 weeks

期刊介绍： Clinical and Molecular Allergy is an open access, peer-reviewed, online journal that publishes research on human allergic and immunodeficient disease (immune deficiency not related to HIV infection/AIDS). The scope of the journal encompasses all aspects of the clinical, genetic, molecular and inflammatory aspects of allergic-respiratory (Type 1 hypersensitivity) and non-AIDS immunodeficiency disorders. However, studies of allergic/hypersensitive aspects of HIV infection/AIDS or drug desensitization protocols in AIDS are acceptable. At the basic science level, this includes original work and reviews on the genetic and molecular mechanisms underlying the inflammatory response.