期刊
CELLS
卷 10, 期 6, 页码 -出版社
MDPI
DOI: 10.3390/cells10061442
关键词
dyskinesia; levodopa; Riluzole; abnormal involuntary movements; Tourette syndrome; epigenetics; DNA methylation; Reduced Representation Bisulfite Sequencing (RRBS)
类别
资金
- FP7-People-2012-ITN, project: TS-Eurotrain [316978]
- COST (European Cooperation in Science and Technology) [CA 15214]
- Merit-prize fellowship of Semmelweis University
- Bolyai Janos research fellowship of the Hungarian Academy of Sciences [BO/00987/16/5]
- Ministry of Human Capacities [UNKP-18-4]
- Baron Munchausen Program of the Institute of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University
- National Research, Development and Innovation Office NKFIH, OTKA grant [132695]
- National Research, Development and Innovation Office [NKFIH] [FK131946]
- Hungarian Academy of Sciences [BO/00730/19/8]
- UNKP-2020 New National Excellence Program of the Ministry for Innovation and Technology from the NKFIH
Dyskinesias are abnormal repetitive involuntary movements caused by dysfunctional neuronal activity. While levodopa-induced dyskinesia has no clinical treatment for Parkinson's disease patients, Riluzole shows potential to improve the phenotype by affecting DNA methylation. The study suggests that Riluzole co-treatment may pinpoint specific methylation targets for potential new druggable targets in Levodopa-Induced Dyskinesia.
Dyskinesias are characterized by abnormal repetitive involuntary movements due to dysfunctional neuronal activity. Although levodopa-induced dyskinesia, characterized by tic-like abnormal involuntary movements, has no clinical treatment for Parkinson's disease patients, animal studies indicate that Riluzole, which interferes with glutamatergic neurotransmission, can improve the phenotype. The rat model of Levodopa-Induced Dyskinesia is a unilateral lesion with 6-hydroxydopamine in the medial forebrain bundle, followed by the repeated administration of levodopa. The molecular pathomechanism of Levodopa-Induced Dyskinesia is still not deciphered; however, the implication of epigenetic mechanisms was suggested. In this study, we investigated the striatum for DNA methylation alterations under chronic levodopa treatment with or without co-treatment with Riluzole. Our data show that the lesioned and contralateral striata have nearly identical DNA methylation profiles. Chronic levodopa and levodopa + Riluzole treatments led to DNA methylation loss, particularly outside of promoters, in gene bodies and CpG poor regions. We observed that several genes involved in the Levodopa-Induced Dyskinesia underwent methylation changes. Furthermore, the Riluzole co-treatment, which improved the phenotype, pinpointed specific methylation targets, with a more than 20% methylation difference relative to levodopa treatment alone. These findings indicate potential new druggable targets for Levodopa-Induced Dyskinesia.
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