Markers of T-cell senescence and physical frailty: insights from Singapore Longitudinal Ageing Studies

IF 4.1 Q2 GERIATRICS & GERONTOLOGY npj aging Pub Date : 2015-09-28 DOI:10.1038/npjamd.2015.5
Tze Pin Ng, Xavier Camous, Ma Shwe Zin Nyunt, Anusha Vasudev, Crystal Tze Ying Tan, Liang Feng, Tamas Fulop, Keng Bee Yap, Anis Larbi
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引用次数: 32

Abstract

Elderly individuals have an eroded immune system but whether immune senescence is implicated with the development of frailty is unknown. The underlying immune mechanisms and the link between markers of senescence and physical frailty is not well established. We explored the association of specific T-cell subset markers of immune differentiation and senescence on CD4+ and CD8+ cells (CD28−, CD27− and CD57+) and the immune risk profile (inverted CD4/CD8 ratio <1) with physical frailty among 421 participants who were frail (N=32), prefrail (N=187) and robust (N=202) in the Singapore Longitudinal Ageing Study cohort. In ordinal logistic regression models relating tertile category rank scores of immune biomarker with frailty status (robust, prefrail and frail), CD8+CD28−CD27+ (odds ratio (OR)=1.35, P=0.013), CD4+CD28−CD27+ (OR=1.29, P=0.025), CD8+CD28− (OR=1.31, P=0.022), and CD4/CD8 ratio (OR=1.27, P=0.026) were positively associated with frailty, controlling for age, sex and multimorbidity. CD4/CD8 ratio less than one was not associated with frailty (OR=0.84, P=0.64). In stepwise multinomial logistic regression controlling for age, sex and comorbidity, only CD8+CD28−CD27+ was the independent predictor of prefrailty: highest tertile of the immune marker significantly predicted prefrailty (versus low tertile, OR=1.72, P=0.037) and frailty (OR=2.56, P=0.06). The study supports the hypothetical role of immune senescence in physical frailty, particularly in regard to the observed loss of CD28 expression from both CD8+ cells and CD4+ cells, but not for CD27 or CD4/CD8 ratio as a marker of senescence. The potential of CD8+CD28−CD27+ as a biological marker of frailty should be further investigated in prospective studies. Declining function in a subset of immune cells may render certain elderly individuals especially weak and prone to hospitalization. As we age, a process called immunosenescence undermines the body''s ability to fight infection and recover from injury. Researchers led by Tze Pin Ng at the National University of Singapore have now found evidence that this process contributes to the increased weakness and overall physiological decline observed among the ''frail'' elderly. The researchers analyzed immune cells collected from 421 elderly Singaporeans, and found that T cells from frail patients tended to lack CD28. This protein is associated with immune function, and its absence is a signature of immunosenescence. Importantly, T-cells from patients who subsequently developed frailty also showed reduced CD28. This suggests a link between immunosenescence and frailty, and may offer a useful predictor for unhealthy aging.
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T 细胞衰老和身体虚弱的标志物:新加坡老龄化纵向研究的启示
老年人的免疫系统受到侵蚀,但免疫衰老是否与体质虚弱的发展有关还不得而知。潜在的免疫机制以及衰老标志物与身体虚弱之间的联系尚未得到很好的证实。我们研究了新加坡老龄化纵向研究队列中 421 名体弱者(32 人)、前期体弱者(187 人)和健壮者(202 人)中 CD4+ 和 CD8+ 细胞上特定 T 细胞亚群免疫分化和衰老标志物(CD28-、CD27- 和 CD57+)以及免疫风险特征(倒 CD4/CD8 比率 <1)与体质虚弱的关系。在将免疫生物标志物的三等分类别等级得分与虚弱状态(健壮、前期虚弱和虚弱)相关的序数逻辑回归模型中,CD8+CD28-CD27+(几率比(OR)=1.35,P=0.013)、CD4+CD28-CD27+(OR=1.29,P=0.025)、CD8+CD28-(OR=1.31,P=0.022)和 CD4/CD8 比值(OR=1.27,P=0.026)与虚弱呈正相关,并控制了年龄、性别和多病症。CD4/CD8 比率小于 1 与虚弱无关(OR=0.84,P=0.64)。在控制年龄、性别和合并症的逐步多项式逻辑回归中,只有 CD8+CD28-CD27+ 是虚弱前期的独立预测因子:免疫标记物的最高三分位数可显著预测虚弱前期(相对于低三分位数,OR=1.72,P=0.037)和虚弱(OR=2.56,P=0.06)。该研究支持免疫衰老在体质虚弱中的假设作用,尤其是观察到 CD8+ 细胞和 CD4+ 细胞中 CD28 表达的丧失,而 CD27 或 CD4/CD8 比值作为衰老标志物的作用则不明显。CD8+CD28-CD27+ 作为衰弱生物学标志物的潜力应在前瞻性研究中进一步调查。免疫细胞亚群功能下降可能会使某些老年人特别虚弱,容易住院。随着年龄的增长,一种叫做免疫衰老的过程会削弱人体抗感染和从损伤中恢复的能力。由新加坡国立大学 Tze Pin Ng 领导的研究人员发现,有证据表明免疫衰老是导致 "体弱 "老人身体更加虚弱和整体生理机能下降的原因之一。研究人员分析了从 421 名新加坡老人身上收集到的免疫细胞,发现体弱病人的 T 细胞往往缺乏 CD28。这种蛋白质与免疫功能有关,它的缺失是免疫衰老的标志。重要的是,随后出现虚弱的患者的 T 细胞也显示出 CD28 的减少。这表明免疫衰老与虚弱之间存在联系,并可能为不健康的衰老提供一个有用的预测指标。
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