Effects of ageing and frailty on circulating monocyte and dendritic cell subsets.

IF 4.1 Q2 GERIATRICS & GERONTOLOGY
Rosanne D Reitsema, Ashok K Kumawat, Bernd-Cornèl Hesselink, Debbie van Baarle, Yannick van Sleen
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Abstract

Ageing is associated with dysregulated immune responses, resulting in impaired resilience against infections and low-grade inflammation known as inflammageing. Frailty is a measurable condition in older adults characterized by decreased health and physical impairment. Dendritic cells (DCs) and monocytes play a crucial role in initiating and steering immune responses. To assess whether their frequencies and phenotypes in the blood are affected by ageing or frailty, we performed a flow cytometry study on monocyte and DC subsets in an immune ageing cohort. We included (n = 15 in each group) healthy young controls (HYC, median age 29 years), healthy older controls (HOC, 73 years) and Frail older controls (76 years). Monocyte subsets (classical, intermediate, non-classical) were identified by CD14 and CD16 expression, and DC subsets (conventional (c)DC1, cDC2, plasmacytoid (p)DC) by CD11c, CD1c, CD141 and CD303 expression. All subsets were checked for TLR2, TLR4, HLA-DR, CD86, PDL1, CCR7 and CD40 expression. We observed a lower proportion of pDCs in HOC compared to HYC. Additionally, we found higher expression of activation markers on classical and intermediate monocytes and on cDC2 in HOC compared to HYC. Frail participants had a higher expression of CD40 on classical and non-classical monocytes compared to the HOC group. We document a substantial effect of ageing on monocytes and DCs. Reduced pDCs in older people may underlie their impaired ability to counter viral infections, whereas enhanced expression of activation markers could indicate a state of inflammageing. Future studies could elucidate the functional consequences of CD40 upregulation with frailty.

Abstract Image

衰老和虚弱对循环单核细胞和树突状细胞亚群的影响。
衰老与免疫反应失调有关,免疫反应失调会导致抗感染和低度炎症(即炎症老化)的能力下降。虚弱是老年人的一种可测量的状况,其特点是健康状况下降和身体受损。树突状细胞(DC)和单核细胞在启动和引导免疫反应方面发挥着至关重要的作用。为了评估它们在血液中的频率和表型是否会受到衰老或虚弱的影响,我们对免疫衰老人群中的单核细胞和树突状细胞亚群进行了流式细胞术研究。我们的研究对象包括(每组 15 人)健康年轻对照组(HYC,中位年龄 29 岁)、健康老年对照组(HOC,73 岁)和老年体弱对照组(76 岁)。单核细胞亚群(经典、中间、非经典)通过 CD14 和 CD16 表达进行鉴定,DC 亚群(传统 (c)DC1、cDC2、类浆细胞 (p)DC)通过 CD11c、CD1c、CD141 和 CD303 表达进行鉴定。我们还检查了所有亚群的 TLR2、TLR4、HLA-DR、CD86、PDL1、CCR7 和 CD40 表达情况。与 HYC 相比,我们观察到 HOC 中 pDC 的比例较低。此外,我们还发现,与 HYC 相比,HOC 中经典单核细胞、中间单核细胞和 cDC2 的活化标志物表达更高。与 HOC 组相比,体弱者的经典和非经典单核细胞中 CD40 的表达更高。我们记录了衰老对单核细胞和 DC 的重大影响。老年人体内 pDCs 的减少可能是其对抗病毒感染能力减弱的原因,而活化标志物表达的增强则可能表明其处于炎症状态。未来的研究可以阐明 CD40 上调对虚弱的功能性影响。
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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CiteScore
8.90
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