Terminally differentiated effector memory T cells associate with cognitive and AD-related biomarkers in an aging-based community cohort.

IF 5.2 2区 医学 Q1 GERIATRICS & GERONTOLOGY Immunity & Ageing Pub Date : 2024-06-12 DOI:10.1186/s12979-024-00443-2
Edric Winford, Jenny Lutshumba, Barbara J Martin, Donna M Wilcock, Gregory A Jicha, Barbara S Nikolajczyk, Ann M Stowe, Adam D Bachstetter
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Abstract

Background and purpose: The immune response changes during aging and the progression of Alzheimer's disease (AD) and related dementia (ADRD). Terminally differentiated effector memory T cells (called TEMRA) are important during aging and AD due to their cytotoxic phenotype and association with cognitive decline. However, it is not clear if the changes seen in TEMRAs are specific to AD-related cognitive decline specifically or are more generally correlated with cognitive decline. This study aimed to examine whether TEMRAs are associated with cognition and plasma biomarkers of AD, neurodegeneration, and neuroinflammation in a community-based cohort of older adults.

Methods: Study participants from a University of Kentucky Alzheimer's Disease Research Center (UK-ADRC) community-based cohort of aging and dementia were used to test our hypothesis. There were 84 participants, 44 women and 40 men. Participants underwent physical examination, neurological examination, medical history, cognitive testing, and blood collection to determine plasma biomarker levels (Aβ42/Aβ40 ratio, total tau, Neurofilament Light chain (Nf-L), Glial Fibrillary Acidic Protein (GFAP)) and to isolate peripheral blood mononuclear cells (PBMCs). Flow cytometry was used to analyze PBMCs from study participants for effector and memory T cell populations, including CD4+ and CD8+ central memory T cells (TCM), Naïve T cells, effector memory T cells (TEM), and effector memory CD45RA+ T cells (TEMRA) immune cell markers.

Results: CD8+ TEMRAs were positively correlated with Nf-L and GFAP. We found no significant difference in CD8+ TEMRAs based on cognitive scores and no associations between CD8+ TEMRAs and AD-related biomarkers. CD4+ TEMRAs were associated with cognitive impairment on the MMSE. Gender was not associated with TEMRAs, but it did show an association with other T cell populations.

Conclusion: These findings suggest that the accumulation of CD8+ TEMRAs may be a response to neuronal injury (Nf-L) and neuroinflammation (GFAP) during aging or the progression of AD and ADRD. As our findings in a community-based cohort were not clinically-defined AD participants but included all ADRDs, this suggests that TEMRAs may be associated with changes in systemic immune T cell subsets associated with the onset of pathology.

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在一个以老龄化为基础的社区队列中,终末分化的效应记忆 T 细胞与认知和注意力缺失症相关的生物标志物有关。
背景和目的:在衰老和阿尔茨海默病(AD)及相关痴呆症(ADRD)进展过程中,免疫反应会发生变化。终末分化的效应记忆 T 细胞(称为 TEMRA)因其细胞毒性表型和与认知能力下降的关系而在衰老和老年痴呆症过程中发挥着重要作用。然而,目前还不清楚TEMRA的变化是专门针对与AD相关的认知能力下降,还是更普遍地与认知能力下降相关。本研究旨在研究 TEMRAs 是否与认知能力以及社区老年人队列中的 AD、神经变性和神经炎症的血浆生物标志物有关:我们利用肯塔基大学阿尔茨海默病研究中心(UK-ADRC)社区老年痴呆症队列中的研究参与者来验证我们的假设。共有 84 名参与者,其中女性 44 人,男性 40 人。参与者接受了体格检查、神经系统检查、病史、认知测试和采血,以确定血浆生物标志物水平(Aβ42/Aβ40比率、总tau、神经丝蛋白轻链(Nf-L)、神经纤维酸性蛋白(GFAP)),并分离外周血单核细胞(PBMC)。流式细胞术用于分析研究参与者外周血单核细胞的效应和记忆 T 细胞群,包括 CD4+ 和 CD8+ 中枢记忆 T 细胞(TCM)、新生 T 细胞、效应记忆 T 细胞(TEM)和效应记忆 CD45RA+ T 细胞(TEMRA)免疫细胞标记:结果:CD8+ TEMRA 与 Nf-L 和 GFAP 呈正相关。我们发现 CD8+ TEMRAs 与认知评分无明显差异,CD8+ TEMRAs 与 AD 相关生物标记物之间也无关联。CD4+ TEMRA 与 MMSE 的认知障碍有关。性别与TEMRAs无关,但与其他T细胞群有关联:这些研究结果表明,CD8+ TEMRAs 的积累可能是对衰老或 AD 和 ADRD 进展过程中神经元损伤(Nf-L)和神经炎症(GFAP)的反应。由于我们在社区队列中的发现并非临床定义的 AD 参与者,而是包括了所有 ADRD,这表明 TEMRAs 可能与病理发作相关的全身免疫 T 细胞亚群的变化有关。
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来源期刊
Immunity & Ageing
Immunity & Ageing GERIATRICS & GERONTOLOGY-IMMUNOLOGY
CiteScore
10.20
自引率
3.80%
发文量
55
期刊介绍: Immunity & Ageing is a specialist open access journal that was first published in 2004. The journal focuses on the impact of ageing on immune systems, the influence of aged immune systems on organismal well-being and longevity, age-associated diseases with immune etiology, and potential immune interventions to increase health span. All articles published in Immunity & Ageing are indexed in the following databases: Biological Abstracts, BIOSIS, CAS, Citebase, DOAJ, Embase, Google Scholar, Journal Citation Reports/Science Edition, OAIster, PubMed, PubMed Central, Science Citation Index Expanded, SCImago, Scopus, SOCOLAR, and Zetoc.
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