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1 The Hatter Institute for
Cardiovascular Studies, Brief renal ischemia-reperfusion is
reported to precondition the myocardium; however, the underlying
mechanisms are unknown. This phenomenon was, therefore, investigated
using an in vivo rabbit model of acute myocardial infarction.
Characterization of the mechanisms involved was performed using the
nonselective adenosine receptor antagonist
8-(p-sulfophenyl)theophylline (8-SPT) and the ATP-sensitive potassium
(KATP) channel blocker sodium 5-hydroxydecanoate (5-HD). Pentobarbital-anesthetized rabbits underwent
a left thoracotomy and pericardiotomy. A laparotomy was then performed
to expose the left renal artery. Animals were either preconditioned
with a 10-min occlusion of the renal artery followed by 10 min of
reperfusion or underwent a 20-min sham period of anesthesia.
Subsequently, the left coronary artery was then occluded for 30 min and
reperfused for 2 h. Infarct-to-risk ratio was limited from 32.7 ± 4.0% (n = 12) in controls to 17.8 ± 3.0% (n = 9;
P = 0.002) in preconditioned hearts.
Protection was abolished by 7.5 mg/kg iv 8-SPT (36.7 ± 3.7%;
n = 6) or 5 mg/kg iv 5-HD (33.1 ± 4.4%; n = 6) administered before
preconditioning. 8-SPT (40.0 ± 4.4%;
n = 6) or 5-HD (40.5 ± 4.2%;
n = 6) did not affect infarct-to-risk
ratio in sham controls. Thus activation of both adenosine receptors and
KATP channels appears to be
involved in acute renal preconditioning of the myocardium.
cardioprotection; remote myocardial preconditioning; sodium
5-hydroxydecanoate; 8-(p-sulfophenyl)theophylline
THE PHENOMENON of ischemic preconditioning (brief
periods of ischemia interspersed with reperfusion) is well
established in the heart (16) and has also been observed in a number of
other organs, including the brain (8), liver (11), and skeletal muscle
(15). There is also limited evidence for increased tolerance to
ischemia in the kidney; however, much of the data are
contradictory, and the profile of protection appears to differ from
preconditioning of the myocardium (20, 21).
Brief coronary artery occlusion has, furthermore, been demonstrated to
precondition the myocardium not only within but also beyond the
perfusion territory of the artery (17), termed "intraorgan" or
"remote" preconditioning. The phenomenon of remote
preconditioning is not, however, unique to the heart because Liauw et
al. (9) have shown that one skeletal muscle can be protected against
ischemia-reperfusion injury by prior ischemic preconditioning
of the contralateral muscle. This evidence has lead to speculation that
ischemic preconditioning of one organ might confer protection on a
remote organ.
Interorgan or remote organ preconditioning of the myocardium was first
described by McClanahan et al. (12) in an open-chest rabbit model of
myocardial infarction. Brief renal artery occlusion followed by a short period of reperfusion was found to limit myocardial infarct size to a similar degree to ischemic preconditioning triggered by brief coronary artery occlusion. This phenomenon has also been observed in rats (4) in which transient ischemia and
reperfusion of either the small intestine or the kidney protected the
myocardium against prolonged ischemia. Although the evidence
for remote organ preconditioning of the myocardium is mounting, there
has been very little investigation of the mechanisms involved.
The aims of this study were to investigate this phenomenon of renal
preconditioning of the myocardium and to characterize the mechansims
involved, using an in vivo rabbit model of myocardial infarction. The
role of two mediators known to be involved in the mechanisms of
myocardial preconditioning, in the rabbit, namely adenosine receptors
(14) and ATP-sensitive potassium
(KATP) channels (5), were
studied in this novel form of protection.
Experimental materials. Sodium
5-hydroxydecanoate (5-HD) and
8-(p-sulfophenyl)theophylline (8-SPT)
were obtained from Research Biochemicals (through Semat, St. Albans,
UK), and both were dissolved in 0.9% wt/vol sodium chloride.
Zinc-cadmium sulfide microspheres (1-10 µm) were from Duke
Scientific (Palo Alto, CA), and 2,3,5-triphenyltetrazolium chloride was
from Sigma (Poole, UK). All other reagents were of analytic quality.
Male New Zealand White rabbits (2.2-3.5 kg body wt) were used for
these studies and were cared for in accordance with UK Home Office
guidelines set out in the Animals (Scientific Procedures) Act 1986.
Experimental procedures. Rabbits were
anesthetized with a combination of 0.15 ml/kg im Hypnorm (contains:
0.315 mg/ml fentanyl citrate and 10 mg/ml fluanisone; Janssen Animal
Health, Petteridge, UK) and 40-50 mg/kg iv pentobarbital sodium.
Surgical anesthesia was maintained by hourly administration of 0.075 ml/kg im Hypnorm and 5-10 mg/kg iv pentobarbital sodium when
required. A tracheotomy was performed, and the animals were
mechanically ventilated with oxygen-supplemented room air at a rate of
56 cycles/min. The right carotid artery was cannulated for
measurement of hemodynamic, arterial blood gas, and pH parameters.
Arterial blood pH was maintained within the range of 7.35-7.50 by
adjustment of the tidal volume. The body core temperature, measured
with a rectal thermometer (T200; Digitron Instrumentation, Hertford,
UK), was carefully maintained at 38.0-38.5°C by means of a
heating pad (Harvard Instruments, Edenbridge, UK).
A left thoracotomy and pericardiotomy were performed, and a 3-0 silk suture (Mersilk W546; Ethicon) was placed around an anterolateral branch of the left coronary artery approximately midway between the
left atrial insertion and the apex. A left laparotomy was then
performed and the left renal artery exposed. A piece of polycotton silk
was passed under the artery to facilitate later retrieval. To prevent
spasm of the exposed renal artery, 0.25-0.5 ml of 2% wt/vol
lidocaine solution was administered locally. Either 7.5 mg/kg 8-SPT
(10) or 5 mg/kg 5-HD (6) was administered by intraveous bolus 10 or 15 min, respectively, before the preconditioning/sham period. Animals then
underwent either a 20-min sham period of anesthesia or 10 min of left
renal artery occlusion followed by 10 min of reperfusion. The renal
artery was occluded 1-2 cm proximal to the kidney using an
atraumatic clip; the polycotton silk was used to gently lift the artery
to facilitate placement of the clip. Successful occlusion was confirmed
visually by a change in the surface color of the left kidney from
pinkish-red to cream; reperfusion was confirmed by blushing of the
previously discolored kidney surface. Ten minutes later the coronary
artery was occluded for 30 min by clamping the ligature with a
polypropylene snare. Occlusion was verified by the appearance of
epicardial cyanosis and S-T segment deviation in the surface electrocardiogram.
Reperfusion was instituted for 2 h by releasing the snare and was
visually confirmed by epicardial blushing, gradual resolution of the
electrocardiogram signal, and the occurrence of reperfusion-induced ventricular premature beats. At the end of reperfusion, 500 IU heparin
sodium were administered intravenously. The animal was administered an
overdose of anesthetic, and the heart was then excised and perfused in
the Langendorff mode with 0.9% wt/vol saline to wash out blood. The
coronary artery ligature was securely tied, and a 5 mg/ml suspension of
fluorescent zinc-cadmium sulfide microspheres, prepared in 0.9% wt/vol
saline, was slowly infused through the aorta to delineate the
myocardial risk zone under ultraviolet light. Hearts were trimmed of
excess tissue, leaving only the left ventricle, frozen at
An additional four rabbits were used to investigate the effects of
increasing doses of adenosine on diastolic blood pressure and heart
rate. Animals were anesthetized, as above, and a catheter was advanced
from the left femoral vein into the vena cava to approximately the
level of the renal veins. Boluses of saline followed by increasing
doses of adenosine (10, 30, 100, and 300 µg/kg) were administered
intravenously, and the diastolic blood pressure and heart rate were
monitored. Blood pressure and heart rate were allowed to return to
baseline between each administration. This dosing regime was performed
twice in each animal.
Experimental treatment groups. Renal
preconditioning protection of the myocardium was evaluated by randomly
assigning rabbits to groups I and
II. The role of adenosine receptors
and KATP channels in
preconditioning was then investigated by random assignment of
additional rabbits to groups III to
VI inclusive, with the addition of
extra sham and preconditioned controls (Fig.
1). Group I was the control sham period corresponding to renal
artery occlusion (sham) before 30 min of ischemia and 2 h of
reperfusion. Group II was renal
preconditioning (PC), which consisted of 10 min of renal
ischemia followed by 10 min of reperfusion before
ischemia-reperfusion. Group
III consisted of sham + 8-SPT (7.5 mg/kg iv) 10 min
before the sham period. Group IV was
PC + 8-SPT (7.5 mg/kg iv) 10 min before renal PC.
Group V was sham + 5-HD (5 mg/kg iv)
15 min before the sham period. Group
VI was PC + 5-HD (5 mg/kg iv) 15 min before renal PC.
ABSTRACT
Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References
INTRODUCTION
Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References
MATERIALS AND METHODS
Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References
18°C for 2-18 h, and then sectioned into 2-mm
transverse sections from apex to base. Slices were incubated in 1%
wt/vol triphenyltetrazolium chloride in phosphate buffer (pH 7.4) at
37°C. Triphenyltetrazolium chloride reacts with dehydrogenases in
viable tissue, producing a red formazan derivative, which is
distinguished from the grey necrotic tissue on fixing with 4% vol/vol
formaldehyde solution. Left ventricular infarct and risk volumes were
determined in a blinded fashion using a computerized planimetric
technique (Kurta, Phoenix, AZ), and the infarct size was expressed as
the percentage of infarction of the risk zone.
View larger version (18K):
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Fig. 1.
Experimental protocol. 5-HD, sodium 5-hydroxydecanoate; 8-SPT,
8-(p-sulfophenyl) theophylline.
Group I, sham period corresponding to
preconditioning (Sham); group II,
renal preconditioning (PC); group III,
Sham + 8-SPT; group IV, PC + 8-SPT;
group V, Sham + 5-HD;
group VI, PC + 5-HD.
Statistical analysis. Differences in
hemodynamic data, arterial blood pressure, core body temperature, and
infarct size among groups were compared by one-factor ANOVA followed by
Fishers protected least-significant difference test. All data are means ± SE. A P 
0.05 was indicative
of a statistically significant difference between groups.
Exclusion criteria. Animals that developed ischemia- or reperfusion-induced ventricular fibrillation (VF) that could not be restored to normal sinus rhythm within 2 min were excluded. Hearts were additionally excluded if the risk or infarct zones were not clearly defined or if the risk volume was <0.4 cm3 or >1.9 cm3.
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RESULTS |
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Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References
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Exclusions. A total of 62 rabbits were used in this study. Thirteen animals were excluded: one due to failure to occlude the renal artery, two due to failure to occlude the coronary artery, two due to failure to reperfuse the coronary artery, one due to severe hypotension, one due to intractible ischemia-induced VF, two due to poor delineation of the risk zone, and four due to a risk zone <0.4 cm3 or >1.9 cm3. Final numbers in the study were therefore 12 sham, 9 renal PC, 6 sham + 8-SPT, 6 PC + 8-SPT, 6 sham + 5-HD, 6 PC + 5-HD, and 4 for the adenosine dose response.
Incidence of ventricular fibrillation. Nine hearts underwent VF during coronary artery occlusion or shortly after reperfusion: three sham, two sham + 8-SPT, two PC + 8-SPT, one sham + 5-HD, and one PC + 5-HD. There was a single incidence of transient reperfusion-induced VF in the sham + 8-SPT group. With the exception of one sham, which developed intractible VF and was excluded (see above), all were converted to normal sinus rhythm within 2 min and were included in the statistical analysis. None of the preconditioned hearts demonstrated VF.
Hemodynamic and temperature data. There were no differences in heart rate, mean arterial blood pressure, rate-pressure product (systolic blood pressure × heart rate), or core body temperature (Table 1) except at baseline for rate-pressure product in the preconditioning group. This resulted from a significantly higher systolic blood pressure; however, there were no differences during ischemia or reperfusion among the groups. The overall similarity in systemic hemodynamic and blood gas parameters, with careful maintenance of core body temperature (38.0-38.5°C) and pH (7.35-7.50), suggests that these factors did not contribute to the significant differences observed in infarct size.
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Infarct data. Myocardial infarct volume was significantly smaller in animals pretreated with renal preconditioning (0.17 ± 0.03 cm3, n = 9) compared with sham controls (0.41 ± 0.07 cm3, n = 12; P < 0.05 by one-factor ANOVA). Neither 7.5 mg/kg 8-SPT (0.53 ± 0.07 cm3; n = 6) nor 5 mg/kg 5-HD (0.57 ± 0.08 cm3; n = 6) alone affected sham control infarct volume. These treatments, however, abolished the infarct volume limitation afforded by renal preconditioning (0.48 ± 0.06 cm3, n = 6, and 0.40 ± 0.07 cm3, n = 6, respectively). When infarct size was expressed as a percentage of the risk zone, renal preconditioning resulted in significantly smaller infarcts (17.8 ± 3.0%) compared with sham controls (32.7 ± 4.0%; P = 0.002 by one-factor ANOVA). This 46% limitation in infarct size is indicative of acute myocardial protection afforded by brief renal ischemia-reperfusion and was abolished by 7.5 mg/kg 8-SPT or 5 mg/kg 5-HD (36.7 ± 3.7 and 33.1 ± 4.4%, respectively). Neither compound alone had any effect on sham control infarct size (40.0 ± 4.4 and 40.5 ± 4.2%, respectively). Figure 2 is a graphical representation of percent infarction within the risk zone. Because mean myocardial risk volume was similar for all six groups (1.0-1.4 cm3), the observed differences in infarct size were not likely to be due to variations in the risk zone.
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Blood pressure. An interesting observation arising from this study was the appearance of a transient drop in diastolic blood pressure (mean drop of 22 ± 0.9 mmHg lasting ~30 s; n = 7) when the renal artery clip was removed to allow reperfusion (Fig. 3). This fall in blood pressure was associated, in the majority of instances, with a small tachycardia (10-20 beats/min). The drop in diastolic blood pressure was abolished by pretreatment with 8-SPT but only attenuated by 5-HD (mean drop of 14 ± 1.5 mmHg; n = 6). The duration of the response, however, was unchanged at ~30 s. The associated tachycardia was also abolished by 8-SPT but was unchanged by 5-HD (Fig. 3).
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The effects of increasing doses of adenosine, administered at the level of the renal veins, were subsequently investigated on the diastolic blood pressure and heart rate. Tachyphylaxis did not occur with increasing doses of adenosine; therefore, blood pressure and heart rate responses were averaged for the two dose-response curves performed in each animal. Saline was found not to alter the blood pressure or heart rate. The effect on diastolic blood pressure produced by the lowest dose of adenosine (10 µg/kg) was indistinguishable from the saline controls, although it did result in a small increase in heart rate. Doses of 30, 100, and 300 µg/kg adenosine produced a dose-dependent decrease in diastolic blood pressure (Fig. 4). Tachycardia, probably reflex in origin, was observed to coincide with the drop in blood pressure, and only at the highest dose of adenosine was this tachycardia preceded by an appreciable bradycardia.
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DISCUSSION |
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Top
Abstract
Introduction
Materials & Methods
Results
Discussion
References
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In this in vivo rabbit model of myocardial infarction, renal preconditioning, instigated by a brief period of left renal artery occlusion followed by reperfusion, limited myocardial infarct size by 46%. This protection was abolished by pretreatment with the nonselective adenosine receptor antagonist 8-SPT or the KATP channel blocker 5-HD before renal preconditioning.
To allow comparison between the treatments, variations in the principal
determinants of infarct size were minimized in the following ways:
1) by excluding risk zones <0.4
cm3 and >1.9
cm3;
2) by expressing infarct size
as a percentage of the risk zone to allow for differences in vascular
anatomy or occlusion site; 3) by
maintaining core body temperature at 38.0-38.5°C,
physiological for the rabbit, since differences of 1°C during
ischemia can markedly affect infarct size (2); and
4) by choosing
the rabbit because it is a noncollateralized species.
Renal preconditioning of the myocardium was first reported by McClanahan et al. (12) in a similar in vivo rabbit model of myocardial infarction. In their study, however, control infarct size (43 ± 3%) was limited to the same degree as coronary preconditioning (renal PC: 11 ± 2%; coronary PC: 8 ± 2%). The reason for the difference in the magnitude of protection between the two studies is unclear, although contemporaneous studies on myocardial preconditioning were not carried out in the present series of experiments. Coronary, mesenteric, and renal ischemic preconditioning of the myocardium in the rat has been shown to be enhanced (coronary and mesenteric) or become apparent (renal) by whole body hypothermia (4). Because core body temperature was not reported by McClanahan et al. (12), perhaps the difference in the magnitude of protection arises from differing temperature conditions. McClanahan et al. (12) and Gho et al. (4) have, moreover, demonstrated the importance of brief intervening reperfusion between the remote organ preconditioning and sustained myocardial ischemia. Protection was lost if the renal or mesenteric artery, respectively, was permanently occluded before myocardial ischemia, suggesting that infarct size limitation required the washout of an endogenous protective factor from the previously ischemic organ.
Potential mechanism for reperfusion-induced drop in blood pressure. A transient drop in diastolic blood pressure on renal artery reperfusion has been previously documented (7). This phenomenon was not observed in sham controls, suggesting that it resulted from the release of an endogenous factor from the ischemic kidney and not from manipulation of the renal artery, vein, or nerve. The drop in blood pressure was abolished by 8-SPT, implying that adenosine mediated this vasodilation. Partial, but significant, attenuation of the fall in blood pressure was noted with 5-HD, alluding to a possible role of KATP channels in the vasodilator response.
Potential mechanisms for renal preconditioning of myocardium. The exact mechanisms by which adenosine and KATP channels mediate renal preconditioning of the myocardium are unclear. Several possibilities warrant consideration including the following. First, adenosine, generated within the ischemic kidney, might be the sole mediator of cardioprotection. Experiments with bolus doses of adenosine showed that ~50 µg/kg iv elicited a fall in blood pressure comparable to that seen immediately on renal artery reperfusion. This implies that the kidney generated at least 100-150 µg of adenosine during the 10 min of ischemia (assuming complete washout on reperfusion). It seems unlikely, however, that this would be sufficient to confer cardioprotection directly, since doses of adenosine as high as 5 mg iv (infused over 5 min) (11) and 25 mg/kg iv (4a) failed to protect rabbit myocardium. Second, adenosine, acting via adenosine receptors within the kidney, might evoke local release of another substance more stable in blood, such as kinins, endothelins, prostaglandins, or renal medullary lipids, which may confer cardioprotection perhaps via a KATP channel-linked mechanism. Third, adenosine, or some substance released by it locally within the kidney, might stimulate renal afferents. A neurogenic mode of action has been alluded to by Gho et al. (4), who prevented mesenteric ischemic preconditioning of the myocardium with the ganglion blocker hexamethonium.
5-HD has been demonstrated to abolish cardioprotection without affecting the action potential duration shortening or vasodilator effects of potassium channel openers (3, 13), which are mediated via sarcolemmal KATP channels. In addition, K+ flux through reconstituted rat heart mitochondrial KATP channels was inhibited by 5-HD (K1/2 = 83 µM, where K1/2 is half-maximal K+ flux) (3). These data suggest that 5-HD is a specific blocker of mitochondrial KATP channels and, therefore, implicates a possible role for these channels in renal preconditioning of the myocardium.
Recent evidence for remote organ preconditioning. As this study was in progress, remote organ preconditioning of the myocardium was further reported. Birnbaum et al. (1) demonstrated that skeletal muscle ischemic preconditioning in the rabbit, elicited by reduction of blood flow with concomitant electrical stimulation of the gastrocnemius muscle, limited myocardial infarct size arising from sustained ischemia. In contrast to all the other studies discussed here, there was no intervening reperfusion between muscle preconditioning and sustained ischemia. Because preconditioning was induced by partial stenosis of the femoral artery, there would, however, have been residual blood flow through the muscle, allowing the potential release of protective mediators into the circulation. Takaoka et al. (18), using a similar rabbit model to ours, reported a comparable limitation of myocardial infarct size by renal preconditoning (controls: 34%, renal PC: 20%, coronary PC: 16%). Coronary or renal preconditioning also diminished the detrimental effects of sustained ischemia on myocardial energy metabolism, determined by intracellular pH, and the concentration of ATP and phosphocreatine. This limitation of infarct size and improvement in myocardial energy metabolism were both abolished by 8-SPT, thus providing the first indication for a role of adenosine receptors in remote organ preconditioning of the myocardium. It was noted in those studies that 8-SPT was administered during the intervening period of reperfusion between preconditioning and sustained ischemia, suggesting that occupation of adenosine receptors by adenosine is necessary during the prolonged myocardial ischemia. In our study, 8-SPT was given before the preconditioning ischemia, implying that adenosine receptors are important for both triggering and mediating remote organ preconditioning of the myocardium, akin to acute coronary preconditioning (19). However, the half-life of 8-SPT, ~45 min, (10) is long enough to block adenosine receptors during both the preconditioning and sustained ischemia.
In summary, renal ischemic preconditioning provided significant protection against sustained myocardial ischemia. The nonselective adenosine receptor antagonist 8-SPT or the KATP channel blocker 5-HD abolished this protection. This study provides the first evidence for the activation of KATP channels, perhaps in the inner mitochondrial membrane, in the mechanism of remote organ preconditioning and supports a role for adenosine receptors in this phenomenon. Further investigation, however, is required to elucidate the precise nature of the involvement of adenosine receptor and KATP channel activation in cardioprotection afforded by remote organ preconditioning.
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ACKNOWLEDGEMENTS |
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T. J. Pell is a recipient of a Glaxo Wellcome studentship. G. F. Baxter is the recipient of a British Heart Foundation personal fellowship (FS 97/001).
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FOOTNOTES |
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The costs of publication of this article were defrayed in part by the payment of page charges. The article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. §1734 solely to indicate this fact.
Address for reprint requests: G. F. Baxter, The Hatter Institute for Cardiovascular Studies, Univ. College London Hospitals & Medical School, Grafton Way, London WC1E 6DB, UK.
Received 24 February 1998; accepted in final form 15 July 1998.
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  M. Shahid, M. Tauseef, K. K. Sharma, and M. Fahim Brief femoral artery ischaemia provides protection against myocardial ischaemia-reperfusion injury in rats: the possible mechanisms Exp Physiol, August 1, 2008; 93(8): 954 - 968. [Abstract] [Full Text] [PDF]
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 L. C. Huffman, S. E. Koch, and K. L. Butler Coronary effluent from a preconditioned heart activates the JAK-STAT pathway and induces cardioprotection in a donor heart Am J Physiol Heart Circ Physiol, January 1, 2008; 294(1): H257 - H262. [Abstract] [Full Text] [PDF]
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M. R. Schmidt, M. Smerup, I. E. Konstantinov, M. Shimizu, J. Li, M. Cheung, P. A. White, S. B. Kristiansen, K. Sorensen, V. Dzavik, et al. Intermittent peripheral tissue ischemia during coronary ischemia reduces myocardial infarction through a KATP-dependent mechanism: first demonstration of remote ischemic perconditioning Am J Physiol Heart Circ Physiol, April 1, 2007; 292(4): H1883 - H1890. [Abstract] [Full Text] [PDF]
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D. A. Liem, M. te Lintel Hekkert, O. C. Manintveld, F. Boomsma, P. D. Verdouw, and D. J. Duncker Myocardium tolerant to an adenosine-dependent ischemic preconditioning stimulus can still be protected by stimuli that employ alternative signaling pathways Am J Physiol Heart Circ Physiol, March 1, 2005; 288(3): H1165 - H1172. [Abstract] [Full Text] [PDF]
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S. B. Kristiansen, O. Henning, R. K. Kharbanda, J. E. Nielsen-Kudsk, M. R. Schmidt, A. N. Redington, T. T. Nielsen, and H. E. Botker Remote preconditioning reduces ischemic injury in the explanted heart by a KATP channel-dependent mechanism Am J Physiol Heart Circ Physiol, March 1, 2005; 288(3): H1252 - H1256. [Abstract] [Full Text] [PDF]
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M. A. Moses, P. D. Addison, P. C. Neligan, H. Ashrafpour, N. Huang, M. Zair, A. Rassuli, C. R. Forrest, G. J. Grover, and C. Y. Pang Mitochondrial KATP channels in hindlimb remote ischemic preconditioning of skeletal muscle against infarction Am J Physiol Heart Circ Physiol, February 1, 2005; 288(2): H559 - H567. [Abstract] [Full Text] [PDF]
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P. D. Addison, P. C. Neligan, H. Ashrafpour, A. Khan, A. Zhong, M. Moses, C. R. Forrest, and C. Y. Pang Noninvasive remote ischemic preconditioning for global protection of skeletal muscle against infarction Am J Physiol Heart Circ Physiol, October 1, 2003; 285(4): H1435 - H1443. [Abstract] [Full Text] [PDF]
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E. W. Dickson, R. J. Tubbs, W. A. Porcaro, W. J. Lee, D. J. Blehar, R. E. Carraway, C. E. Darling, and K. Przyklenk Myocardial preconditioning factors evoke mesenteric ischemic tolerance via opioid receptors and KATP channels Am J Physiol Heart Circ Physiol, July 1, 2002; 283(1): H22 - H28. [Abstract] [Full Text] [PDF]
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D. A. Liem, P. D. Verdouw, H. Ploeg, S. Kazim, and D. J. Duncker Sites of action of adenosine in interorgan preconditioning of the heart Am J Physiol Heart Circ Physiol, July 1, 2002; 283(1): H29 - H37. [Abstract] [Full Text] [PDF]
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 B. O'Rourke Myocardial KATP Channels in Preconditioning Circ. Res., November 10, 2000; 87(10): 845 - 855. [Abstract] [Full Text] [PDF]
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R. G. Schoemaker and C. L. van Heijningen Bradykinin mediates cardiac preconditioning at a distance Am J Physiol Heart Circ Physiol, May 1, 2000; 278(5): H1571 - H1576. [Abstract] [Full Text] [PDF]
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E. W. Dickson, M. Lorbar, W. A. Porcaro, R. A. Fenton, C. P. Reinhardt, A. Gysembergh, and K. Przyklenk Rabbit heart can be "preconditioned" via transfer of coronary effluent Am J Physiol Heart Circ Physiol, December 1, 1999; 277(6): H2451 - H2457. [Abstract] [Full Text] [PDF]
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 L. M. Schwiebert, W. C. Rice, B. A. Kudlow, A. L. Taylor, and E. M. Schwiebert Extracellular ATP signaling and P2X nucleotide receptors in monolayers of primary human vascular endothelial cells Am J Physiol Cell Physiol, February 1, 2002; 282(2): C289 - C301. [Abstract] [Full Text] [PDF]
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