The role of nitric oxide and cell adhesion molecules on the microcirculation in ischaemia-reperfusion

被引：220

作者：

Lefer, AM ^{[1
]}

Lefer, DJ ^{[1
]}

机构：

[1] TULANE UNIV, SCH MED, DEPT MED, CARDIOL SECT, NEW ORLEANS, LA 70112 USA

来源：

CARDIOVASCULAR RESEARCH | 1996年 / 32卷 / 04期

关键词：

neutrophils; nitric oxide; endothelium; cell adhesion molecules; selectins; reperfusion; microcirculation;

D O I：

10.1016/S0008-6363(96)00073-9

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

The microcirculation undergoes a profound degree of endothelial dysfunction within minutes (i.e., 2.5 to 5 min) following reperfusion of ischaemic vasculature. This has been documented in the coronary and mesenteric microcirculation. The endothelial dysfunction is characterized by a loss in basal and agonist-mediated nitric oxide (NO) produced by the vascular endothelium. The loss of NO results in upregulation of cell adhesion molecules (CAMs) particularly P-selectin 10-20 min following reperfusion, Thus, CAM upregulation renders the endothelium sticky, and a marked degree of leukocyte adherence (particularly neutrophils) occurs 20 min following reperfusion. This enhanced involvement of neutrophils leads to neutrophil infiltration into the underlying tissue (e.g., myocardium) within 2-3 h of reperfusion, The infiltration of neutrophils leads to reperfusion injury (i.e., necrosis) which is significant at 3 h but becomes profound at 4.5 h following reperfusion. Cardiac necrosis can be significantly attenuated by treatment with NO, an organic NO donor, L-arginine, or specific blockers of CAMs given just prior to reperfusion. This approach is a promising one for a variety of types of reperfusion injury.

引用

页码：743 / 751

页数：9

共 70 条

[61] ADHESION RECEPTORS OF THE IMMUNE-SYSTEM [J].

SPRINGER, TA .

NATURE, 1990, 346 (6283) :425-434

[62] TIME COURSE OF ENDOTHELIAL DYSFUNCTION AND MYOCARDIAL INJURY DURING MYOCARDIAL-ISCHEMIA AND REPERFUSION IN THE CAT [J].

TSAO, PS ;

AOKI, N ;

LEFER, DJ ;

JOHNSON, G ;

LEFER, AM .

CIRCULATION, 1990, 82 (04) :1402-1412

[63] TIME COURSE AND MECHANISM OF ENDOTHELIAL DYSFUNCTION IN ISOLATED ISCHEMIC-PERFUSED AND HYPOXIC-PERFUSED RAT HEARTS [J].

TSAO, PS ;

LEFER, AM .

AMERICAN JOURNAL OF PHYSIOLOGY, 1990, 259 (06) :H1660-H1666

[64] INVOLVEMENT OF PLATELET ENDOTHELIAL-CELL ADHESION MOLECULE-1 IN NEUTROPHIL RECRUITMENT IN-VIVO [J].

VAPORCIYAN, AA ;

DELISSER, HM ;

YAN, HC ;

MENDIGUREN, II ;

THOM, SR ;

JONES, ML ;

WARD, PA ;

ALBELDA, SM .

SCIENCE, 1993, 262 (5139) :1580-1582

[65] THE ROLE OF L-ARGININE IN AMELIORATING REPERFUSION INJURY AFTER MYOCARDIAL-ISCHEMIA IN THE CAT [J].

WEYRICH, AS ;

MA, XL ;

LEFER, AM .

CIRCULATION, 1992, 86 (01) :279-288

[66] TIME-COURSE OF CORONARY VASCULAR ENDOTHELIAL ADHESION MOLECULE EXPRESSION DURING REPERFUSION OF THE ISCHEMIC FELINE MYOCARDIUM [J].

WEYRICH, AS ;

BUERKE, M ;

ALBERTINE, KH ;

LEFER, AM .

JOURNAL OF LEUKOCYTE BIOLOGY, 1995, 57 (01) :45-55

[67] PHYSIOLOGICAL CONCENTRATIONS OF NITRIC-OXIDE DO NOT ELICIT AN ACUTE NEGATIVE INOTROPIC EFFECT IN UNSTIMULATED CARDIAC-MUSCLE [J].

WEYRICH, AS ;

MA, XL ;

BUERKE, M ;

MUROHARA, T ;

ARMSTEAD, VE ;

LEFER, AM ;

NICOLAS, JM ;

THOMAS, AP ;

LEFER, DJ ;

VINTENJOHANSEN, J .

CIRCULATION RESEARCH, 1994, 75 (04) :692-700

[68] INVIVO NEUTRALIZATION OF P-SELECTIN PROTECTS FELINE HEART AND ENDOTHELIUM IN MYOCARDIAL-ISCHEMIA AND REPERFUSION INJURY [J].

WEYRICH, AS ;

MA, XL ;

LEFER, DJ ;

ALBERTINE, KH ;

LEFER, AM .

JOURNAL OF CLINICAL INVESTIGATION, 1993, 91 (06) :2620-2629

[69]

WINQUIST R, 1990, CIRCULATION, V82, P701

[70]

WINQUIST RJ, 1992, CIRCULATION, V86, P79

← 1 2 3 4 5 6 7 →