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Novel Nasal Epithelial Cell Markers of Parkinson's Disease Identified Using Cells Treated with alpha-Synuclein Preformed Fibrils

Authors
Kim, H[Kim, Hyojung]Kang, SJ[Kang, Seok-Jae]Jo, YM[Jo, Young Mi]Park, S[Park, Sanggyu]Yun, SP[Yun, Seung Pil]Lee, YS[Lee, Yun-Song]Kim, HT[Kim, Hee-Tae]Lee, NE[Lee, Nae-Eung]Kim, YS[Kim, Yong-Sang]Cho, SH[Cho, Seok Hyun]Lee, Y[Lee, Yunjong]
Issue Date
Jul-2020
Publisher
MDPI
Keywords
nasal epithelial cell model; Parkinson' s disease; RPMI-2650 cells; olfactory biomarker; alpha-synuclein preformed fibril; olfactory dysfunction
Citation
JOURNAL OF CLINICAL MEDICINE, v.9, no.7, pp.1 - 15
Journal Title
JOURNAL OF CLINICAL MEDICINE
Volume
9
Number
7
Start Page
1
End Page
15
URI
https://scholarworks.bwise.kr/skku/handle/2021.sw.skku/3979
DOI
10.3390/jcm9072128
ISSN
2077-0383
Abstract
Parkinson's disease (PD) is the most common neurodegenerative movement disorder, characterized by olfactory dysfunction in the early stages. alpha-Synuclein pathologies in the olfactory organs are shown to spread to the brain through the nose-brain axis. We first developed a nasal epithelial PD cellular model by treating RPMI-2650 cells with alpha-synuclein preformed fibrils (PFF). Upon uptake of PFF, RPMI-2650 cells showed mitochondrial proteome alteration and downregulation of parkin, which has previously been identified as a nasal biomarker of PD. Functional cluster analysis of differentially expressed genes in RPMI-2650 cells revealed various pathways affected by alpha-synuclein pathology, including the detection of chemical stimulus involved in sensory perception, olfactory receptor activity, and sensory perception of smell. Among genes that were most affected, we validated, by real-time quantitative PCR, the downregulation ofMAP3K8,OR10A4,GRM2,OR51B6, andOR9A2,as well as upregulation ofIFIT1B,EPN1, OR1D5, LCN, and OTOL1in PFF-treated RPMI-2650 cells. Subsequent analyses of clinical samples showed a downregulation ofOR10A4andOR9A2transcripts and an upregulation ofIFIT1Bin cells isolated from the nasal fluid of PD patients, as compared to those from the controls (cutoff value = 0.5689 forOR9A2,with 72.4% sensitivity and 75% specificity, and 1.4658 forIFIT1B,with 81.8% sensitivity and 77.8% specificity). Expression levels of these nasal PD markers were not altered in nasal fluid cells from SWEDD (scans without evidence of dopaminergic deficits) patients with PD-like motor symptoms. These nasal markers were significantly altered in patients of PD with hyposmia compared to the control hyposmic subjects. Our results validated the alpha-synuclein-treated nasal epithelial cell model to identify novel biomarkers for PD and suggest the utility of olfactory transcripts, along with olfactory dysfunction, in the diagnosis of PD.
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