DNA methylation changes in genes involved in inflammation and depression in fibromyalgia: a pilot study
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De Gruyter
Abstract
Objectives: The present pilot study aims to investigate
DNA methylation changes of genes related to fibromyalgia
(FM) development and its main comorbid symptoms,
including sleep impairment, inflammation, depression
and other psychiatric disorders. Epigenetic modifications
might trigger or perpetuate complex interplay between
pain transduction/transmission, central pain processing
and experienced stressors in vulnerable individuals.
Methods: We conducted DNA methylation analysis by
targeted bisulfite NGS sequencing testing differential
methylation in 112 genomic regions from leukocytes of
eight women with FM and their eight healthy sisters as
controls.
Results: Tests for differentially methylated regions and
cytosines brought focus on the GRM2 gene, encoding the metabotropic glutamate receptor2. The slightly increased
DNA methylation observed in the GRM2 region of FM patients
may confirm the involvement of the glutamate
pathway in this pathological condition. Logistic regression
highlighted the simultaneous association of methylation
levels of depression and inflammation-related genes
with FM.
Conclusions: Altogether, the results evidence the glutamate
pathway involvement in FM and support the idea that
a combination of methylated and unmethylated genes
could represent a risk factor to FM or its consequence, more
than single genes. Further studies on the identified biomarkers
could contribute to unravel the causative underlying
FM mechanisms, giving reliable directions to
research, improving the diagnosis and effective therapies
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Gerra, M., Carnevali, D., Pedersen, I., Donnini, C., Manfredini, M., González-Villar, A., Triñanes, Y., Pidal-Miranda, M., Arendt-Nielsen, L. & Carrillo-de-la-Peña, M. (2021). DNA methylation changes in genes involved in inflammation and depression in fibromyalgia: a pilot study. Scandinavian Journal of Pain, 21(2), 372-383
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https://doi.org/10.1515/sjpain-2020-0124Sponsors
This study was supported by Spanish Government Funding (Ministerio de Economía y Competitividad: grant PSI2013-45818-R). The genotyping service was carried out at CEGEN-PRB3-ISCIII; it is supported by grant PT17/0019, of the PE I + D + i 2013–2016, funded by ISCIII and ERDF. MCG and LAN are part of the Center for Neuroplasticity and Pain (CNAP) which is supported by the Danish National Research Foundation (DNRF121)
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© 2020 Maria Carla Gerra et al., published by De Gruyter. This work is licensed under the Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/)








