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Transcriptional analysis of peripheral memory T cells reveals Parkinson's disease-specific gene signatures.

Rekha DhanwaniJoão Rodrigues Lima-JuniorAshu SethiJohn PhamGregory P WilliamsApril FrazierYaqian XuAmy W AmaraDavid G StandaertJennifer G GoldmanIrene LitvanRoy N AlcalayBjoern PetersDavid L SulzerCecilia S Lindestam ArlehamnAlessandro Sette
Published in: NPJ Parkinson's disease (2022)
Parkinson's disease (PD) is a multi-stage neurodegenerative disorder with largely unknown etiology. Recent findings have identified PD-associated autoimmune features including roles for T cells. To further characterize the role of T cells in PD, we performed RNA sequencing on PBMC and peripheral CD4 and CD8 memory T cell subsets derived from PD patients and age-matched healthy controls. When the groups were stratified by their T cell responsiveness to alpha-synuclein (α-syn) as a proxy for an ongoing inflammatory autoimmune response, the study revealed a broad differential gene expression profile in memory T cell subsets and a specific PD associated gene signature. We identified significant enrichment of transcriptomic signatures previously associated with PD, including for oxidative stress, phosphorylation, autophagy of mitochondria, cholesterol metabolism and inflammation, and the chemokine signaling proteins CX3CR1, CCR5, and CCR1. In addition, we identified genes in these peripheral cells that have previously been shown to be involved in PD pathogenesis and expressed in neurons, such as LRRK2, LAMP3, and aquaporin. Together, these findings suggest that features of circulating T cells with α-syn-specific responses in PD patients provide insights into the interactive processes that occur during PD pathogenesis and suggest potential intervention targets.
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