Affiliation:
1. Cardiovascular Physiology Core Department of Medicine Brigham and Women’s Hospital Harvard Medical School Boston MA
2. Epidemiology Unit Rambam Health Care Center Haifa Israel
3. Eliachar Research Laboratory Galilee Medical Center Nahariya Israel
4. CVPath Institute Gaithersburg MD
5. Department of Developmental Biology and Cancer Research Institute of Medical Research Israel‐Canada Hebrew University of Jerusalem–Hadassah Medical School Jerusalem Israel
6. Stanford University School of Medicine Cardiovascular Institute Stanford CA
7. Department of Vascular Surgery Sheba Medical Center Sackler Faculty of Medicine Tel Aviv University Tel Aviv Israel
Abstract
Background
Marfan syndrome (
MFS
) is a genetically transmitted connective tissue disorder characterized by aortic root dilatation, dissection, and rupture. Molecularly,
MFS
pathological features have been shown to be driven by increased angiotensin
II
in the aortic wall. Using an angiotensin
II
–driven aneurysm mouse model, we have recently demonstrated that local inhibition of leptin activity restricts aneurysm formation in the ascending and abdominal aorta. As we observed de novo leptin synthesis in the ascending aortic aneurysm wall of patients with MFS, we hypothesized that local counteracting of leptin activity in
MFS
may also prevent aortic cardiovascular complications in this context.
Methods and Results
Fbn1
C1039G/+
mice underwent periaortic application of low‐dose leptin antagonist at the aortic root. Treatment abolished medial degeneration and prevented increase in aortic root diameter (
P
<0.001). High levels of leptin, transforming growth factor β1, Phosphorylated Small mothers against decapentaplegic 2, and angiotensin‐converting enzyme 1 observed in saline‐treated
MFS
mice were downregulated in leptin antagonist–treated animals (
P
<0.01,
P
<0.05,
P
<0.001, and
P
<0.001, respectively). Leptin and angiotensin‐converting enzyme 1 expression levels in left ventricular cardiomyocytes were also decreased (
P
<0.001) and coincided with prevention of left ventricular hypertrophy and aortic and mitral valve leaflet thickening (
P
<0.01 and
P
<0.05, respectively) and systolic function preservation.
Conclusions
Local, periaortic application of leptin antagonist prevented aortic root dilatation and left ventricular valve remodeling, preserving left ventricular systolic function in an
MFS
mouse model. Our results suggest that local inhibition of leptin may constitute a novel, stand‐alone approach to prevent
MFS
aortic root aneurysms and potentially other similar angiotensin
II
–driven aortic pathological features.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Cardiology and Cardiovascular Medicine
Cited by
7 articles.
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