Down syndrome (DS) is caused by the presence of part or an entire extra copy of chromosome 21, a phenomenon that can cause a wide spectrum of clinically defined phenotypes of the disease. Most of the clinical signs of DS are typical of the ageing process including dysregulation of immune system. Beyond the causative genetic defect, DS persons display epigenetic alterations, particularly aberrant DNA methylation patterns that can contribute to the heterogeneity of the disease. In the present work we investigated the levels of 5-hydroxymethylcytosine (5hmC) and of the TET dioxygenase enzymes, which are involved in DNA demethylation processes and are often deregulated in pathological conditions as well as in ageing. Analyses were carried out on peripheral blood mononuclear cells of DS volunteers enrolled in the context of the MARK-AGE study, a large-scale cross-sectional population study with subjects representing the general population in eight European countries. We observed a decrease of 5hmC, TET1 and other components of the DNA methylation/demethylation machinery in DS subjects, indicating that aberrant DNA methylation patterns in DS, which may have consequences on the transcriptional status of immune cells, may be due to a global disturbance of methylation control in DS.

DNA hydroxymethylation levels are altered in blood cells from Down syndrome persons enrolled in the MARK-AGE project / Ciccarone, Fabio; Valentini, Elisabetta; Malavolta, Marco; Zampieri, Michele; Bacalini, MARIA GIULIA; Calabrese, Roberta; Guastafierro, Tiziana; Reale, Anna; Franceschi, Claudio; Capri, Miriam; Breusing, Nicolle; Grune, Tilman; Moreno villanueva, María; Bürkle, Alexander; Caiafa, Paola. - In: JOURNALS OF GERONTOLOGY SERIES A-BIOLOGICAL SCIENCES AND MEDICAL SCIENCES. - ISSN 1079-5006. - STAMPA. - 73:6(2018), pp. 737-744. [10.1093/gerona/glx198]

DNA hydroxymethylation levels are altered in blood cells from Down syndrome persons enrolled in the MARK-AGE project

CICCARONE, FABIO
;
VALENTINI, ELISABETTA;ZAMPIERI, Michele;BACALINI, MARIA GIULIA;CALABRESE, ROBERTA;GUASTAFIERRO, Tiziana;REALE, Anna;CAIAFA, Paola
2018

Abstract

Down syndrome (DS) is caused by the presence of part or an entire extra copy of chromosome 21, a phenomenon that can cause a wide spectrum of clinically defined phenotypes of the disease. Most of the clinical signs of DS are typical of the ageing process including dysregulation of immune system. Beyond the causative genetic defect, DS persons display epigenetic alterations, particularly aberrant DNA methylation patterns that can contribute to the heterogeneity of the disease. In the present work we investigated the levels of 5-hydroxymethylcytosine (5hmC) and of the TET dioxygenase enzymes, which are involved in DNA demethylation processes and are often deregulated in pathological conditions as well as in ageing. Analyses were carried out on peripheral blood mononuclear cells of DS volunteers enrolled in the context of the MARK-AGE study, a large-scale cross-sectional population study with subjects representing the general population in eight European countries. We observed a decrease of 5hmC, TET1 and other components of the DNA methylation/demethylation machinery in DS subjects, indicating that aberrant DNA methylation patterns in DS, which may have consequences on the transcriptional status of immune cells, may be due to a global disturbance of methylation control in DS.
2018
5-hydroxymethylcytosine; TET enzymes;, DNA methylation; aging
01 Pubblicazione su rivista::01a Articolo in rivista
DNA hydroxymethylation levels are altered in blood cells from Down syndrome persons enrolled in the MARK-AGE project / Ciccarone, Fabio; Valentini, Elisabetta; Malavolta, Marco; Zampieri, Michele; Bacalini, MARIA GIULIA; Calabrese, Roberta; Guastafierro, Tiziana; Reale, Anna; Franceschi, Claudio; Capri, Miriam; Breusing, Nicolle; Grune, Tilman; Moreno villanueva, María; Bürkle, Alexander; Caiafa, Paola. - In: JOURNALS OF GERONTOLOGY SERIES A-BIOLOGICAL SCIENCES AND MEDICAL SCIENCES. - ISSN 1079-5006. - STAMPA. - 73:6(2018), pp. 737-744. [10.1093/gerona/glx198]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1014587
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