Effect of a critical coronary stenosis on myocardial neutrophil accumulation during ischemia and early reperfusion in dogs

In many experimental models of ischemia and reperfusion, reperfusion is performed abruptly, allowing full reactive hyperemia to occur. In the clinical setting, however, reperfusion after thrombolysis is often limited by residual stenosis. Some experimental models attempt to mimic this situation with...

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Veröffentlicht in:	Circulation (New York, N.Y.) N.Y.), 1989-12, Vol.80 (6), p.1805-1815
Hauptverfasser:	RICHARD, V. J, BROOKS, S. E, JENNINGS, R. B, REIMER, K. A
Format:	Artikel
Sprache:	eng
Schlagworte:	550601 - Medicine- Unsealed Radionuclides in Diagnostics ALBUMINS ANIMAL TISSUES ANIMALS ARTERIES BETA DECAY RADIOISOTOPES BIOLOGICAL ACCUMULATION Biological and medical sciences BIOLOGICAL MATERIALS BLOOD BLOOD CELLS BLOOD FLOW BLOOD VESSELS BODY BODY FLUIDS Cardiology. Vascular system CARDIOVASCULAR DISEASES CARDIOVASCULAR SYSTEM Constriction, Pathologic - pathology CORONARIES Coronary Circulation Coronary heart disease Coronary Vessels - pathology DAYS LIVING RADIOISOTOPES DISEASES DOGS ELECTRON CAPTURE RADIOISOTOPES Female HEART Hyperemia - prevention & control INDIUM 111 INDIUM ISOTOPES Indium Radioisotopes INTERMEDIATE MASS NUCLEI IODINE 125 IODINE ISOTOPES ISCHEMIA ISOMERIC TRANSITION ISOTOPES ISOTOPES LEUKOCYTES Male MAMMALS MATERIALS Medical sciences MINUTES LIVING RADIOISOTOPES MUSCLES Myocardial Reperfusion - methods Myocardial Reperfusion Injury - pathology Myocardial Reperfusion Injury - prevention & control MYOCARDIUM Myocardium - pathology NEUTROPHILS Neutrophils - physiology NUCLEI ODD-EVEN NUCLEI ORGANIC COMPOUNDS ORGANS PERFUSED TISSUES PROTEINS RADIOISOTOPES RADIOLOGY AND NUCLEAR MEDICINE Time Factors TISSUES VASCULAR DISEASES VERTEBRATES
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Zusammenfassung:	In many experimental models of ischemia and reperfusion, reperfusion is performed abruptly, allowing full reactive hyperemia to occur. In the clinical setting, however, reperfusion after thrombolysis is often limited by residual stenosis. Some experimental models attempt to mimic this situation with a "critical stenosis" (defined as a coronary constriction sufficient to abolish reactive hyperemia without altering baseline flow). The purpose of this study was to determine whether preventing reactive hyperemia during the initial phase of reperfusion would modify the transmural distribution of myocardial blood flow or the myocardial accumulation of polymorphonuclear leukocytes (PMNs). The left circumflex artery was occluded for 90 minutes and then reperfused for 60 minutes in anesthetized, open-chest dogs. Autologous PMNs were isolated, labeled with 111In, and reinjected 1 hour before coronary occlusion. 125I-labeled albumin was injected simultaneously to correct for 111In associated with plasma proteins and to permit calculation of the number of PMNs in the inner, middle, and outer thirds of nonischemic and ischemic-reperfused tissue. The presence of a critical stenosis abolished reactive hyperemia during the first 5 minutes of reperfusion, but did not substantially affect blood flow measured after 55 minutes of reperfusion. In both groups, there was a significant accumulation of PMNs in all layers of the ischemic-reperfused bed compared with the nonischemic bed, and the magnitude of this PMN accumulation was not altered by the presence of a critical stenosis. Moreover, infarct size, estimated by triphenyl tetrazolium chloride (TTC) loss after 60 minutes of reperfusion, was not affected by the presence of a critical stenosis. Thus, the presence of a critical stenosis abolished the hyperemic blood flow after reperfusion but did not influence the early PMN response to ischemia and reperfusion or the early loss of TTC staining.
ISSN:	0009-7322 1524-4539
DOI:	10.1161/01.CIR.80.6.1805