Immune responses to oligomeric α-synuclein in Parkinson’s disease peripheral blood mononuclear cells

免疫系统 外周血单个核细胞 免疫学 帕金森病 医学 细胞因子 神经退行性变 生物 病理 疾病 体外 生物化学
作者
Ana Florencia Vega-Benedetti,Clara Porcedda,Tommaso Ercoli,Giuliana Fusco,Chiara Burgaletto,Rita Pillai,Francesca Palmas,Anna Cantone,Fabrizio Angius,Paolo Solla,Alfonso De Simone,Giuseppina Cantarella,Cesarina Giallongo,Valeria Sogos,Giovanni Defazio,Anna R. Carta
出处
期刊:Journal of Neurology [Springer Nature]
卷期号:271 (9): 5916-5929
标识
DOI:10.1007/s00415-024-12554-3
摘要

Parkinson's disease displays clinical heterogeneity, presenting with motor and non-motor symptoms. Heterogeneous phenotypes, named brain-first and body-first, may reflect distinct α-synuclein pathology starting either in the central nervous system or in the periphery. The immune system plays a prominent role in the central and peripheral pathology, with misfolded α-synuclein being placed at the intersection between neurodegeneration and inflammation. Here, we characterized the inflammatory profile and immune-phenotype of peripheral blood mononuclear cells (PBMCs) from Parkinson's disease patients upon stimulation with α-synuclein monomer or oligomer, and investigated relationships of immune parameters with clinical scores of motor and non-motor symptoms. Freshly isolated PBMCs from 21 Parkinson's disease patients and 18 healthy subjects were exposed in vitro to α-synuclein species. Cytokine/chemokine release was measured in the culture supernatant by Multiplex Elisa. The immune-phenotype was studied by FACS-flow cytometry. Correlation analysis was computed between immune parameters and parkinsonian motor and non-motor scales. We found that Parkinson's disease patients exhibited a dysregulated PBMC-cytokine profile, which remained unaltered after exposure to α-synuclein species and correlated with both motor and non-motor severity, with a strong correlation observed with olfactory impairment. Exposure of PBMCs from healthy controls to α-synuclein monomer/oligomer increased the cytokine/chemokine release up to patient's values. Moreover, the PBMCs immune phenotype differed between patients and controls and revealed a prominent association of the Mos profile with olfactory impairment, and of NK profile with constipation. Results suggest that a deranged PBMC-immune profile may reflect distinct clinical subtypes and would fit with the recent classification of Parkinson's disease into peripheral-first versus brain-first phenotype.

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