Altered T cell reactivity to β-amyloid-related antigens in early Alzheimer’s disease

Author:

Rickenbach ChiaraORCID,Mallone AnnaORCID,Häusle Lars,Frei Larissa,Seiter Sarina,Sparano ColinORCID,Kirabali TunahanORCID,Blennow Kaj,Zetterberg Henrik,Ferretti Maria Teresa,Kulic Luka,Hock Christoph,Nitsch Roger M.,Treyer ValerieORCID,Gietl AntonORCID,Gericke ChristophORCID

Abstract

AbstractThere is growing evidence that the adaptive immune system and neurodegenerative Alzheimer’s disease (AD) are intertwined in multiple ways. Recent studies have reported alterations of the adaptive immune system in early AD stages, such as preclinical AD and mild cognitive impairment (MCI) due to AD. However, the identity of specific antigenic targets and whether the respective response is beneficial or detrimental during disease progression are still open questions. Herein, we describe cross-sectional analyses of blood and cerebrospinal fluid from three different study populations covering early AD stages. We employed high-dimensional mass cytometry, single-cell RNA-sequencing,in vitroT cell secretome analysis, and antigen presentation assays to achieve a comprehensive characterization of adaptive immune cell populations. Our results show that subjects at the stage of asymptomatic, preclinical AD can mount a CD4+T helper cell response towards β- amyloid peptide and display an early enrichment of cytotoxic CD8+effector/TEMRA cells in CSF, combined with a less immunosuppressive gene signature of peripheral regulatory T cells. Conversely, in MCI due to AD, we observed increased frequencies of CD8+effector/TEMRA cells in the periphery, characterized by a pro-inflammatory gene expression profile and an overall decrease in antigen responsiveness. Our results demonstrate the complexity of adaptive immune changes in early AD and suggest that it may be beneficial in the preclinical stage to promote specific CD4+T cell responses, while in MCI it may be important to therapeutically target CD8+T cell responses if these prove to be harmful.

Publisher

Cold Spring Harbor Laboratory

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