Literature DB >> 29992529

MTOR Pathway-Based Discovery of Genetic Susceptibility to L-DOPA-Induced Dyskinesia in Parkinson's Disease Patients.

Núria Martín-Flores1,2, Rubén Fernández-Santiago3,4,5, Francesa Antonelli4, Catalina Cerquera4,6, Verónica Moreno4, Maria Josep Martí3,4,5, Mario Ezquerra3,4,5, Cristina Malagelada7,8.   

Abstract

Dyskinesia induced by L-DOPA administration (LID) is one of the most invalidating adverse effects of the gold standard treatment restoring dopamine transmission in Parkinson's disease (PD). However, LID manifestation in parkinsonian patients is variable and heterogeneous. Here, we performed a candidate genetic pathway analysis of the mTOR signaling cascade to elucidate a potential genetic contribution to LID susceptibility, since mTOR inhibition ameliorates LID in PD animal models. We screened 64 single nucleotide polymorphisms (SNPs) mapping to 57 genes of the mTOR pathway in a retrospective cohort of 401 PD cases treated with L-DOPA (70 PD with moderate/severe LID and 331 with no/mild LID). We performed classic allelic, genotypic, and epistatic analyses to evaluate the association of individual or combinations of SNPs with LID onset and with LID severity after initiation of L-DOPA treatment. As for the time to LID onset, we found significant associations with SNP rs1043098 in the EIF4EBP2 gene and also with an epistatic interaction involving EIF4EBP2 rs1043098, RICTOR rs2043112, and PRKCA rs4790904. For LID severity, we found significant association with HRAS rs12628 and PRKN rs1801582 and also with a four-loci epistatic combination involving RPS6KB1 rs1292034, HRAS rs12628, RPS6KA2 rs6456121, and FCHSD1 rs456998. These findings indicate that the mTOR pathway contributes genetically to LID susceptibility. Our study could help to identify the most susceptible PD patients to L-DOPA in order to prevent the appearance of early and/or severe LID in a future. This information could also be used to stratify PD patients in clinical trials in a more accurate way.

Entities:  

Keywords:  Dyskinesia; Epistasia; L-DOPA; Parkinson’s disease; Single nucleotide polymorphism; mTOR

Mesh:

Substances:

Year:  2018        PMID: 29992529     DOI: 10.1007/s12035-018-1219-1

Source DB:  PubMed          Journal:  Mol Neurobiol        ISSN: 0893-7648            Impact factor:   5.590


  52 in total

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2.  Modification of Parkinsonism--chronic treatment with L-dopa.

Authors:  G C Cotzias; P S Papavasiliou; R Gellene
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3.  Dopa-decarboxylase gene polymorphisms affect the motor response to L-dopa in Parkinson's disease.

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Journal:  Parkinsonism Relat Disord       Date:  2013-10-24       Impact factor: 4.891

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Review 5.  Priming for l-dopa-induced dyskinesia in Parkinson's disease: a feature inherent to the treatment or the disease?

Authors:  Agnès Nadjar; Charles R Gerfen; Erwan Bezard
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6.  mTOR inhibition alleviates L-DOPA-induced dyskinesia in parkinsonian rats.

Authors:  Mickael Decressac; Anders Björklund
Journal:  J Parkinsons Dis       Date:  2013       Impact factor: 5.568

7.  Aberrant restoration of spines and their synapses in L-DOPA-induced dyskinesia: involvement of corticostriatal but not thalamostriatal synapses.

Authors:  Yiyue Zhang; Gloria E Meredith; Nasya Mendoza-Elias; David J Rademacher; Kuei Y Tseng; Kathy Steece-Collier
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8.  Polymorphisms of Dopamine Receptor Genes and Risk of L-Dopa-Induced Dyskinesia in Parkinson's Disease.

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9.  Rapamycin activation of 4E-BP prevents parkinsonian dopaminergic neuron loss.

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Journal:  Front Oncol       Date:  2013-07-24       Impact factor: 6.244

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Review 2.  The Rodent Models of Dyskinesia and Their Behavioral Assessment.

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Review 4.  Challenges and Future Prospects of Precision Medicine in Psychiatry.

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5.  Identification of Potential Core Genes in Parkinson's Disease Using Bioinformatics Analysis.

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6.  Discovery of levodopa-induced dyskinesia-associated genes using genomic studies in patients and Drosophila behavioral analyses.

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  6 in total

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