Abnormal remodeling of atherosclerotic plaques can lead to rupture, acute myocardial infarction, and death. Enhancement of plaque extracellular matrix (ECM) may improve plaque morphology and stabilize lesions. Here, we demonstrate that chronic administration of LNA-miR-29 into an atherosclerotic mouse model improves indices of plaque morphology. This occurs due to upregulation of miR-29 target genes of the ECM (col1A and col3A) resulting in reduced lesion size, enhanced fibrous cap thickness, and reduced necrotic zones. Sustained LNA-miR-29 treatment did not affect circulating lipids, blood chemistry, or ECM of solid organs including liver, lung, kidney, spleen, or heart. Collectively, these data support the idea that antagonizing miR-29 may promote beneficial plaque remodeling as an independent approach to stabilize vulnerable atherosclerotic lesions.SynopsisAntagonizing miR-29 decreases atherosclerotic lesion size and improves indices of plaque stability. LNA-miR-29 treatment increases ECM components in the plaque compared to adjacent non-plaque vessel, and treated VSMC secretome analysis indicates that ECM proteins are highly regulated by miR-29.Antagonism of miR-29 reduces atherosclerotic lesion size. Reducing miR-29 improves indices of plaque stability. Manipulating miR-29 invitro influences the VSMC secretome.
Chronic miR-29 antagonism promotes favorable plaque remodeling in atherosclerotic mice / Ulrich, V.; Rotllan, N.; Araldi, E.; Luciano, A.; Skroblin, P.; Abonnenc, M.; Perrotta, P.; Yin, X.; Bauer, A.; Leslie, K. L.; Zhang, P.; Aryal, B.; Montgomery, R. L.; Thum, T.; Martin, K.; Suarez, Y.; Mayr, M.; Fernandez-Hernando, C.; Sessa, W. C.. - In: EMBO MOLECULAR MEDICINE. - ISSN 1757-4676. - 8:6(2016), pp. 643-653. [10.15252/emmm.201506031]
Chronic miR-29 antagonism promotes favorable plaque remodeling in atherosclerotic mice
Araldi E.;
2016-01-01
Abstract
Abnormal remodeling of atherosclerotic plaques can lead to rupture, acute myocardial infarction, and death. Enhancement of plaque extracellular matrix (ECM) may improve plaque morphology and stabilize lesions. Here, we demonstrate that chronic administration of LNA-miR-29 into an atherosclerotic mouse model improves indices of plaque morphology. This occurs due to upregulation of miR-29 target genes of the ECM (col1A and col3A) resulting in reduced lesion size, enhanced fibrous cap thickness, and reduced necrotic zones. Sustained LNA-miR-29 treatment did not affect circulating lipids, blood chemistry, or ECM of solid organs including liver, lung, kidney, spleen, or heart. Collectively, these data support the idea that antagonizing miR-29 may promote beneficial plaque remodeling as an independent approach to stabilize vulnerable atherosclerotic lesions.SynopsisAntagonizing miR-29 decreases atherosclerotic lesion size and improves indices of plaque stability. LNA-miR-29 treatment increases ECM components in the plaque compared to adjacent non-plaque vessel, and treated VSMC secretome analysis indicates that ECM proteins are highly regulated by miR-29.Antagonism of miR-29 reduces atherosclerotic lesion size. Reducing miR-29 improves indices of plaque stability. Manipulating miR-29 invitro influences the VSMC secretome.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
