miRNA-based signatures in cerebrospinal fluid as potential diagnostic tools for early stage Parkinson’s disease

Santos, Márcia Cristina Teixeira dos; Barreto-Sanz, Miguel Arturo; Correia, Bruna Renata S; Bell, Rosie; Widnall, Catherine; Perez, Luis Tosar; Berteau, Caroline; Schulte, Claudia; Scheller, D.; Berg, Daniela; Maetzler, Walter; Galante, Pedro A. F.; Costa, André Nogueira da

doi:10.18632/oncotarget.24736

Cited by 106 publications

(87 citation statements)

References 60 publications

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“…Of the 8 miRNAs that were differentially expressed between iPD and controls, 4 (50%) have been previously identified as deregulated in PD. These were miR-7-5p, 71 miR-22-3p, [72][73][74] miR-124-3p, 75 and miR-433-3p. 76 Another interesting finding is that the miRNAs found deregulated in genetic versus iPD cases were very different.…”

Section: Discussionmentioning

confidence: 99%

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

et al. 2019

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Background A minimally invasive test for early detection and monitoring of Parkinson's disease (PD) is a highly unmet need for drug development and planning of patient care. Blood plasma represents an attractive source of biomarkers. MicroRNAs (miRNAs) are conserved noncoding RNA molecules that serve as posttranscriptional regulators of gene expression. As opposed to ubiquitously expressed miRNAs that control house‐keeping processes, brain‐enriched miRNAs regulate diverse aspects of neuron development and function. These include neuron‐subtype specification, axonal growth, dendritic morphogenesis, and spine density. Backed by a large number of studies, we now know that the differential expression of neuron‐enriched miRNAs leads to brain dysfunction. Objectives The aim was to identify subsets of brain‐enriched miRNAs with diagnostic potential for familial and idiopathic PD as well as specify the molecular pathways deregulated in PD. Methods Initially, brain‐enriched miRNAs were selected based on literature review and validation studies in human tissues. Subsequently, real‐time reverse transcription polymerase chain reaction was performed in the plasma of 100 healthy controls and 99 idiopathic and 53 genetic (26 alpha‐synucleinA53T and 27 glucocerebrosidase) patients. Statistical and bioinformatics analyses were carried out to pinpoint the diagnostic biomarkers and deregulated pathways, respectively. Results An explicit molecular fingerprint for each of the 3 PD cohorts was generated. Although the idiopathic PD fingerprint was different from that of genetic PD, the molecular pathways deregulated converged between all PD subtypes. Conclusions The study provides a group of brain‐enriched miRNAs that may be used for the detection and differentiation of PD subtypes. It has also identified the molecular pathways deregulated in PD. © 2019 International Parkinson and Movement Disorder Society

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Section: Discussionmentioning

confidence: 99%

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

et al. 2019

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“…Shortcomings for biomarker research are the RNA input requirements for sequencing protocols as well as the still relatively high costs of NGS. Some studies demonstrate that downscaling is possible without losing sensitivity and specificity ( Burgos et al, 2013 , 2014 ; Rao et al, 2013 ; dos Santos et al, 2018 ). As NGS is still a relatively new technique and the solutions for small RNA sequencing are continuously improved, it is likely that this technique will be more widely available in the future.…”

Section: Sources Technical Considerations and Biomarker Potential Ofmentioning

confidence: 99%

“…Thereof, 6 miRNAs were further validated based on their involvement in related signaling pathways: miR-1, miR-19b-3p showed decreased expression in PD, while miR-153, miR-409-3p, miR-10a-5p, and let-7g-3p were found upregulated. A recent study reported that 5 miRNAs were able to differentiate between early stage PD and healthy controls: miR-151a-3p and let-7f-5p were up-regulated in PD CSF, whereas miR-27a-3p, miR-125a-5p, and miR-423-5p were significantly decreased ( dos Santos et al, 2018 ). The different studies performed with total CSF or CSF-exosomes show no overlapping results, even though the cohorts were of a comparable size.…”

Section: Circulating Mirnas As Biomarkers In Parkinson’s Diseasementioning

confidence: 99%

Circulating miRNAs as Diagnostic Biomarkers for Parkinson’s Disease

et al. 2018

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Parkinson’s disease (PD) is the second most common neurodegenerative disorder worldwide. Its main neuropathological hallmarks are the degeneration of dopaminergic neurons in the substantia nigra and alpha-synuclein containing protein inclusions, called Lewy Bodies. The diagnosis of idiopathic PD is still based on the assessment of clinical criteria, leading to an insufficient diagnostic accuracy. Additionally, there is no biomarker available allowing the prediction of the disease course or monitoring the response to therapeutic approaches. So far, protein biomarker candidates such as alpha-synuclein have failed to improve diagnosis of PD. Circulating microRNAs (miRNAs) in body fluids are promising biomarker candidates for PD, as they are easily accessible by non- or minimally-invasive procedures and changes in their expression are associated with pathophysiological processes relevant for PD. Advances in miRNA analysis methods resulted in numerous recent publications on miRNAs as putative biomarkers. Here, we discuss the applicability of different body fluids as sources for miRNA biomarkers, highlight technical aspects of miRNA analysis and give an overview on published studies investigating circulating miRNAs as biomarker candidates for diagnosis of PD and other Parkinsonian syndromes.

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“…53 Another study demonstrated that miR-423-5p in cerebrospinal fluid can be selected as one of the members of Parkinson's biomarker panel. 54 In the current study, we truncated the 3ʹUTR of the GRIN1 gene, and initially confirmed the potential functional sequence of the 3ʹ regulatory region of the GRIN1 gene by means of the luciferase reporter assay. Although bioinformatics tools showed the presence of multiple miRNA binding sites in the +295 bp -+ 497 bp region, including miR-212-5p, miR-324-3p and miR-326, further overexpression experiments did not directly demonstrate the regulatory effect of these miRNAs on GRIN1 gene expression.…”

Section: Dovepressmentioning

confidence: 67%

<p>Functional Analysis of the 3ʹ Untranslated Region of the Human <em>GRIN1</em> Gene in Regulating Gene Expression in vitro</p>

Liu

Jinghua

et al. 2020

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Purpose: Abnormal expression of the NR1 subunit of the N-methyl-d-aspartate (NMDA) receptor may potentially increase the susceptibility to neuropsychiatric diseases. The purpose of this study was to investigate the functional sequence of the 3ʹUTR of the human GRIN1 gene, which encodes the GluN1 receptor to determine the effect on the expression of GluN1 receptor. Methods: We transferred seven recombinant pmirGLO recombinant vectors containing the 3ʹUTR truncated fragment of the GRIN1 gene into HEK-293, SK-N-SH, and U87 cell lines and compared the relative fluorescence intensity of adjacent length fragments. The TargetScan database was used to predict miRNAs. Then, miRNA mimics/inhibitors were co-transfected into the three cell lines with the 3ʹUTR of GRIN1 (pmirGLO-GRIN1), to investigate their influence on GRIN1 gene expression. Results: Compared with the pmirGLo-Basic vector, the relative fluorescence intensity of the complete GRIN1 gene 3ʹUTR recombinant sequence −27 bp-+1284 bp (the next base of the stop codon is +1) was significantly decreased in all three cell lines. The relative fluorescence intensities were significantly different between −27 bp-+294 bp and −27 bp-+497 bp regions, and between −27 bp-+708 bp and −27 bp-+907 bp regions. According to the prediction of the TargetScan database and analysis, miR-212-5p, miR-324-3p and miR-326 may bind to +295 bp-+497 bp, while miR-491-5p may bind to +798 bp-+907 bp. After co-transfection of miRNA mimic/inhibitor or mimic/inhibitor NC with a recombinant vector in the 3ʹUTR region of GRIN1 gene, we found that has-miR-491-5p inhibited GRIN1 expression significantly in all three cell lines, while has-miR-326 inhibitor upregulated GRIN1 expression in HEK-293 and U87 cells. Conclusion: miR-491-5p may bind to the 3ʹUTR of the GRIN1 gene (+799 bp-+805 bp, the next base of the stop codon is +1) and down-regulate gene expression in HEK-293, SK-N-SH, and U87 cell lines, which implicates a potential role of miR-491-5p in central nervous system diseases.

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miRNA-based signatures in cerebrospinal fluid as potential diagnostic tools for early stage Parkinson’s disease

Cited by 106 publications

References 60 publications

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

Circulating Brain‐Enriched MicroRNAs for Detection and Discrimination of Idiopathic and Genetic Parkinson's Disease

Circulating miRNAs as Diagnostic Biomarkers for Parkinson’s Disease

<p>Functional Analysis of the 3ʹ Untranslated Region of the Human <em>GRIN1</em> Gene in Regulating Gene Expression in vitro</p>

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