Common signatures of differential microRNA expression in Parkinson’s and Alzheimer’s disease brains

Author:

Dobricic Valerija1,Schilling Marcel1,Farkas Ildiko2,Gveric Djordje O2,Ohlei Olena1,Schulz Jessica1,Middleton Lefkos34,Gentleman Steve M5,Parkkinen Laura6,Bertram Lars17ORCID,Lill Christina M138

Affiliation:

1. Lübeck Interdisciplinary Platform for Genome Analytics (LIGA), University of Lübeck , 23562 Lübeck , Germany

2. Multiple Sclerosis and Parkinson’s Tissue Bank, Imperial College London , London W12 0NN , UK

3. Ageing and Epidemiology Unit (AGE), School of Public Health, Imperial College London , London W6 8RF , UK

4. Public Health Directorate, Imperial College NHS Healthcare Trust , London W6 8RF , UK

5. Department of Brain Sciences, Hammersmith Hospital campus, Imperial College London , London W12 0HS , UK

6. Nuffield Department of Clinical Neurosciences, Oxford Parkinson’s Disease Centre, University of Oxford , Oxford OX3 9DU , UK

7. Department of Psychology, University of Oslo , 0373 Oslo , Norway

8. Institute of Epidemiology and Social Medicine, University of Münster , 48149 Münster , Germany

Abstract

Abstract Dysregulation of microRNA gene expression has been implicated in many neurodegenerative diseases, including Parkinson’s disease. However, the individual dysregulated microRNAs remain largely unknown. Previous meta-analyses have highlighted several microRNAs being differentially expressed in post-mortem Parkinson’s disease and Alzheimer's disease brains versus controls, but they were based on small sample sizes. In this study, we quantified the expression of the most compelling Parkinson’s and Alzheimer’s disease microRNAs from these meta-analyses (‘candidate miRNAs’) in one of the largest Parkinson’s/Alzheimer’s disease case–control post-mortem brain collections available (n = 451), thereby quadruplicating previously investigated sample sizes. Parkinson’s disease candidate microRNA hsa-miR-132-3p was differentially expressed in our Parkinson’s (P = 4.89E−06) and Alzheimer’s disease samples (P = 3.20E−24) compared with controls. Alzheimer’s disease candidate microRNAs hsa-miR-132-5p (P = 4.52E−06) and hsa-miR-129-5p (P = 0.0379) were differentially expressed in our Parkinson’s disease samples. Combining these novel data with previously published data substantially improved the statistical support (α = 3.85E−03) of the corresponding meta-analyses, clearly implicating these microRNAs in both Parkinson’s and Alzheimer’s disease. Furthermore, hsa-miR-132-3p/-5p (but not hsa-miR-129-5p) showed association with α-synuclein neuropathological Braak staging (P = 3.51E−03/P = 0.0117), suggesting that hsa-miR-132-3p/-5p play a role in α-synuclein aggregation beyond the early disease phase. Our study represents the largest independent assessment of recently highlighted candidate microRNAs in Parkinson’s and Alzheimer’s disease brains, to date. Our results implicate hsa-miR-132-3p/-5p and hsa-miR-129-5p to be differentially expressed in both Parkinson’s and Alzheimer’s disease, pinpointing shared pathogenic mechanisms across these neurodegenerative diseases. Intriguingly, based on publicly available high-throughput sequencing of RNA isolated by cross-linking immunoprecipitation data, hsa-miR-132 may interact with SNCA messenger RNA in the human brain, possibly pinpointing novel therapeutic approaches in fighting Parkinson’s disease.

Funder

Deutsche Forschungsgemeinschaft

Cure Alzheimer’s Fund

Brain Bank

Imperial College London

Parkinson’s UK

The Oxford Brain Bank

Medical Research Council

Brains for Dementia Research

Alzheimer Society and Alzheimer Research UK

NIHR Oxford Biomedical Research Centre

Michael J. Fox Foundation

Publisher

Oxford University Press (OUP)

Subject

General Earth and Planetary Sciences,General Environmental Science

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