Renin-sensitive microRNAs correlate with atherosclerosis plaque progression
J Deiuliis, G Mihai, J Zhang, C Taslim… - Journal of Human …, 2014 - nature.com
Journal of Human Hypertension, 2014•nature.com
Recent trials with inhibition of the renin–angiotensin–aldosterone system (RAAS) in patients
with established atherosclerosis have been equivocal. MicroRNAs (miRs) are known to
affect multiple pathways relevant to atherosclerosis, including RAAS. We postulated that the
use of a direct renin antagonist would result in differential regulation of miRs. We examined
monocyte miR expression before and after treatment with renin antagonist, Aliskiren, in
patients with established cardiovascular disease as part of a prospective, single-center …
with established atherosclerosis have been equivocal. MicroRNAs (miRs) are known to
affect multiple pathways relevant to atherosclerosis, including RAAS. We postulated that the
use of a direct renin antagonist would result in differential regulation of miRs. We examined
monocyte miR expression before and after treatment with renin antagonist, Aliskiren, in
patients with established cardiovascular disease as part of a prospective, single-center …
Abstract
Recent trials with inhibition of the renin–angiotensin–aldosterone system (RAAS) in patients with established atherosclerosis have been equivocal. MicroRNAs (miRs) are known to affect multiple pathways relevant to atherosclerosis, including RAAS. We postulated that the use of a direct renin antagonist would result in differential regulation of miRs. We examined monocyte miR expression before and after treatment with renin antagonist, Aliskiren, in patients with established cardiovascular disease as part of a prospective, single-center, randomized, double-blind and placebo-controlled clinical trial (NCT01417104). After screening, patients (mean age 62±3 years) were randomized to placebo or Aliskiren. Three-dimensional dark-blood magnetic resonance imaging assessment of atherosclerosis in the thoracic and abdominal aorta was conducted at baseline and at study completion (19–36 weeks). MiR expression arrays were performed on RNA from peripheral blood mononuclear cells collected at baseline and 12 weeks following randomization to placebo or Aliskiren and showed that hsa-miR-106b-5p, 27a-3p and 18b-5p were significantly downregulated with Aliskiren. Baseline expression of these miRs positively correlated with normalized total wall volume in subjects taking Aliskiren (miR-106b, R= 0.62; miR-27a, R= 0.63; miR-18b, R= 0.77; P< 0.05). Hsa-miR-106b-5p, 27a-3p and 18b-5p may represent pathway-specific adaptations to renin inhibition relevant to atherosclerosis.
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