RAGE Blockade Stabilizes Established Atherosclerosis in Diabetic Apolipoprotein E-null Mice

Overview

Journal Circulation

Specialty Cardiology & Vascular Diseases

Date 2002 Nov 27

PMID 12451010

Citations 197

Authors

Loredana G Bucciarelli

Thoralf Wendt

Wu Qu

Yan Lu

Evanthia Lalla

Ling Ling Rong

Mouza T Goova

Bernhard Moser

Thomas Kislinger

Daniel C Lee

Yogita Kashyap

David M Stern

Ann Marie Schmidt

Affiliations

Soon will be listed here.

Abstract

Background: Previous studies suggested that blockade of RAGE in diabetic apolipoprotein (apo) E-null mice suppressed early acceleration of atherosclerosis. A critical test of the potential applicability of RAGE blockade to clinical settings was its ability to impact established vascular disease. In this study, we tested the hypothesis that RAGE contributed to lesion progression in established atherosclerosis in diabetic apoE-null mice.

Methods And Results: Male apoE-null mice, age 6 weeks, were rendered diabetic with streptozotocin or treated with citrate buffer. At age 14 weeks, certain mice were killed or treated with once-daily murine soluble RAGE or albumin; all mice were killed at age 20 weeks. Compared with diabetic mice at age 14 weeks, albumin-treated animals displayed increased atherosclerotic lesion area and complexity. In diabetic mice treated with sRAGE from age 14 to 20 weeks, lesion area and complexity were significantly reduced and not statistically different from those observed in diabetic mice at age 14 weeks. In parallel, decreased parameters of inflammation and mononuclear phagocyte and smooth muscle cell activation were observed.

Conclusions: RAGE contributes not only to accelerated lesion formation in diabetic apoE-null mice but also to lesion progression. Blockade of RAGE may be a novel strategy to stabilize atherosclerosis and vascular inflammation in established diabetes.

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