identification of circulating micrornas for the differential diagnosis of parkinson’s disease and multiple system atrophy.

identification of circulating micrornas for the differential diagnosis of parkinson’s disease and multiple system atrophy.

;Annamaria eVallelunga;Marco eRagusa;Stefania eDi Mauro;Tommaso eIannitti;Manuela ePilleri;Roberta eBiundo;Luca eWeis;Cinzia eDi Pietro;Angela eDe Iuliis;Alessandra eNicoletti;Mario eZappia;Michele ePurrello;Angelo eAntonini
macromolecular bioscience 2014 Vol. 8 pp. -
230
evallelunga2014frontiersidentification

Abstract

Background. Parkinson's disease (PD) is a progressive neurodegenerative disorder which may be misdiagnosed with atypical conditions such as Multiple System Atrophy (MSA), due to overlapping clinical features. MicroRNAs (miRNAs) are small noncoding RNAs with a key role in post-transcriptional gene regulation. We hypothesized that identification of a distinct set of circulating miRNAs (cmiRNAs) could distinguish patients affected by PD from MSA and healthy individuals. Results. Using TaqMan Low Density Array technology, we analysed 754 miRNAs and found 9 cmiRNAs differentially expressed in PD and MSA patients compared to healthy controls. We also validated a set of 4 differentially expressed cmiRNAs in PD and MSA patients versus controls. More specifically, miR-339-5p was downregulated, whereas miR-223*, miR-324-3p and mir-24 were upregulated in both diseases. We found cmiRNAs specifically deregulated in PD (downregulation of miR-30c and miR-148b) and in MSA (upregulation of miR-148b). Finally, comparing MSA and PD, we identified 3 upregulated cmiRNAs in MSA serum (miR-24, miR-34b, miR-148b). Conclusions. Our results suggest that cmiRNA signatures discriminate PD from MSA patients and healthy controls and may be considered specific, non-invasive biomarkers for differential diagnosis.

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