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CD4+ Regulatory and Effector/Memory T Cell Subsets Profile Motor Dysfunction in Parkinson’s Disease

免疫系统 T细胞 疾病 免疫学 效应器 帕金森病 免疫失调 队列 医学 生物 内科学
作者
Jessica A. Hutter Saunders,Katherine A. Estes,Lisa M. Kosloski,Heather E. Allen,Kathryn Dempsey,Diego Torres‐Russotto,Jane L. Meza,Pamela M. Santamaria,John M. Bertoni,Daniel L. Murman,Hesham Ali,David G. Standaert,R. Lee Mosley,Howard E. Gendelman
出处
期刊:Journal of Neuroimmune Pharmacology [Springer Nature]
卷期号:7 (4): 927-938 被引量:277
标识
DOI:10.1007/s11481-012-9402-z
摘要

Animal models and clinical studies have linked the innate and adaptive immune system to the pathology of Parkinson's disease (PD). Despite such progress, the specific immune responses that influence disease progression have eluded investigators. Herein, we assessed relationships between T cell phenotype and function with PD progression. Peripheral blood lymphocytes from two separate cohorts, a discovery cohort and a validation cohort, totaling 113 PD patients and 96 age- and environment-matched caregivers were examined by flow cytometric analysis and T cell proliferation assays. Increased effector/memory T cells (Tem), defined as CD45RO+ and FAS+ CD4+ T cells and decreased CD31+ and α4β7+ CD4+ T cells were associated with progressive Unified Parkinson's Disease Rating Scale III scores. However, no associations were seen between immune biomarkers and increased age or disease duration. Impaired abilities of regulatory T cells (Treg) from PD patients to suppress effector T cell function was observed. These data support the concept that chronic immune stimulation, notably Tem activation and Treg dysfunction is linked to PD pathobiology and disease severity, but not disease duration. The association of T cell phenotypes with motor symptoms provides fresh avenues for novel biomarkers and therapeutic designs.

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