Affiliation:
1. Division of Cardiology, Mount Sinai and University Health Network Hospitals, Toronto, Canada
2. Department of Pharmacology and Toxicology, University of Toronto, Canada
3. Medizinische Klinik, University Medical Center Mainz, Germany
Abstract
Background
It is well established that acute ischemic preconditioning (
IPC
) protects against ischemia–reperfusion (
IR
) injury; however, the effectiveness of repeated
IPC
exposure has not been extensively investigated. We aimed to determine whether daily
IPC
episodes provide continued protection from
IR
injury in a human forearm model, and the role of cyclooxygenase‐2 in these responses.
Methods and Results
Thirty healthy volunteers were randomized to participate in 2 of 3 protocols (
IR
alone, 1‐day
IPC
, 7‐day
IPC
) in an operator‐blinded, crossover design. Subjects in the
IR
alone protocol underwent flow‐mediated dilation (
FMD
) measurements pre‐ and post‐
IR
(15′ upper‐arm ischemia and 15′ reperfusion). The 1‐day
IPC
protocol involved
FMD
measurements before and after 1 episode of
IPC
(3 cycles of 5′ upper‐arm ischemia and 5′ reperfusion) and
IR
. Day 7 of the 7‐day
IPC
protocol was identical to the 1‐day
IPC
protocol but was preceded by single daily episodes of
IPC
for 6 days prior. During each protocol, subjects received a 7‐day treatment of either the cyclooxygenase‐2 inhibitor celecoxib or placebo. Pre‐
IR FMD
was similar between groups.
IR
alone reduced
FMD
post‐
IR
(placebo, Δ
FMD
: −4.4±0.7%; celecoxib, Δ
FMD
: −5.0±0.5%). One‐day
IPC
completely prevented this effect (placebo, Δ
FMD
: −1.1±0.6%; celecoxib, Δ
FMD
: 0.0±0.7%;
P
<0.0001). Similarly, 7‐day
IPC
demonstrated persistent endothelial protection post‐
IR
(placebo, Δ
FMD
: −0.9±0.9%; celecoxib, Δ
FMD
: 0.0±0.8%;
P
<0.0001,
P
<0.0001 for
ANOVA
effect of
IPC
protocol). Celecoxib did not alter responses to
IR
in any protocol.
Conclusions
Daily episodes of
IPC
provide sustained protection from
IR
‐induced endothelial dysfunction in humans through a mechanism that appears cyclooxygenase‐2‐independent.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Cardiology and Cardiovascular Medicine
Cited by
29 articles.
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