RAGE and Modulation of Ischemic Injury in the Diabetic Myocardium

A. M. Schmidt; Aikawa; Brownlee; C. Strauch; Ceriello; Constien; Cosentino; D. R. Sell; Dimmeler; F. Song; Feng; Harja; Hofmann; Horie; Jaffe; Kislinger; Kubota; L. G. Bucciarelli; Lehto; Levine; Li; M. Kaneko; Marfella; Molina y Vedia; Nagai; Park; R. Ananthakrishnan; R. Ramasamy; RONG; S. F. Yan; Sakaguchi; Schleicher; Schmidt; Sell; SELL; Shehadeh; Smith; Taguchi; Thirunavukkarasu; Tsoporis; Tsoporis; V. M. Monnier; Wang; Wendt; Wu; Y. C. Hwang; Yokoyama; Yue

RAGE and Modulation of Ischemic Injury in the Diabetic Myocardium

Authors: A. M. Schmidt
Aikawa
Brownlee
C. Strauch
Ceriello
Constien
Cosentino
D. R. Sell
Dimmeler
F. Song
Feng
Harja
Hofmann
Horie
Jaffe
Kislinger
Kubota
L. G. Bucciarelli
Lehto
Levine
Li
M. Kaneko
Marfella
Molina y Vedia
Nagai
Park
R. Ananthakrishnan
R. Ramasamy
RONG
S. F. Yan
Sakaguchi
Schleicher
Schmidt
Sell
SELL
Shehadeh
Smith
Taguchi
Thirunavukkarasu
Tsoporis
Tsoporis
V. M. Monnier
Wang
Wendt
Wu
Y. C. Hwang
Yokoyama
Yue
Publication date
Publisher: American Diabetes Association
Doi

Abstract

OBJECTIVE—Subjects with diabetes experience an increased risk of myocardial infarction and cardiac failure compared with nondiabetic age-matched individuals. The receptor for advanced glycation end products (RAGE) is upregulated in diabetic tissues. In this study, we tested the hypothesis that RAGE affected ischemia/reperfusion (I/R) injury in the diabetic myocardium. In diabetic rat hearts, expression of RAGE and its ligands was enhanced and localized particularly to both endothelial cells and mononuclear phagocytes

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