Additive contribution of microRNA-34a/b/c to human arterial ageing and atherosclerosis

Preclinical data suggest that the ageing-induced miR-34a regulates vascular senescence. Herein we sought to assess whether the miR-34 family members miR-34a, miR-34b and miR-34c are involved in human arterial disease. Expression levels of miR-34a/b/c were quantified by TaqMan assay in peripheral blo...

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Veröffentlicht in:Atherosclerosis 2021-06, Vol.327, p.49-58
Hauptverfasser: Gatsiou, Aikaterini, Georgiopoulos, Georgios, Vlachogiannis, Nikolaos I., Pfisterer, Larissa, Fischer, Ariane, Sachse, Marco, Laina, Ageliki, Bonini, Francesca, Delialis, Dimitrios, Tual-Chalot, Simon, Zormpas, Eleftherios, Achangwa, Rawlings, Jiang, Longchang, Kontogiannis, Christos, Patras, Raphael, Hermeking, Heiko, Zeiher, Andreas M., Stamatelopoulos, Kimon, Dimmeler, Stefanie, Stellos, Konstantinos
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Sprache:eng
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Zusammenfassung:Preclinical data suggest that the ageing-induced miR-34a regulates vascular senescence. Herein we sought to assess whether the miR-34 family members miR-34a, miR-34b and miR-34c are involved in human arterial disease. Expression levels of miR-34a/b/c were quantified by TaqMan assay in peripheral blood mononuclear cells (PBMCs) derived from a consecutive cohort of 221 subjects who underwent cardiovascular risk assessment and thorough vascular examination for aortic stiffness and extent of arterial atherosclerosis. High miR-34a was independently associated with the presence of CAD [OR (95%C.I.): 3.87 (1.56–9.56); p = 0.003] and high miR-34c with the number of diseased arterial beds [OR (95%C.I.): 1.88 (1.034–3.41); p = 0.038], while concurrent high expression of miR-34-a/c or all three miR-34a/b/c was associated with aortic stiffening (miR-34a/c: p = 0.022; miR-34a/b/c: p = 0.041) and with the extent of atherosclerosis [OR (95%C.I.) for number of coronary arteries [miR-34a/c: 3.29 (1.085–9.95); miR-34a/b/c: 6.06 (1.74–21.2)] and number of diseased arterial beds [miR-34a/c: 3.51 (1.45–8.52); miR-34a/b/c: 2.89 (1.05–7.92)] after controlling for possible confounders (p 
ISSN:0021-9150
1879-1484
DOI:10.1016/j.atherosclerosis.2021.05.005