Engler R L, Dahlgren M D, Morris D D, Peterson M A, Schmid-Schönbein G W
Am J Physiol. 1986 Aug;251(2 Pt 2):H314-23. doi: 10.1152/ajpheart.1986.251.2.H314.
Recent evidence indicates that leukocytes (LEU) are large, stiff, viscous cells that naturally adhere to vascular endothelium. Their broad role in the early myocardial microvascular response to acute ischemia was suggested by 1) the role of leukocyte capillary plugging in the no-reflow phenomenon, 2) resistance increases in skeletal muscle with LEU infusions, and 3) salvage of ischemic myocardium by anti-LEU agents. We perfused the coronary circulation under matched, controlled conditions with whole blood or granulocyte-depleted whole blood. During 1 h of ischemia (left anterior descending occlusion) circumflex perfusion pressure was servocontrolled to a constant value. In whole blood-perfused hearts, flow measured by the radiolabeled microsphere method decreased in endocardium from 0.12 +/- 0.05 at 5 min of ischemia to 0.09 +/- 0.04 ml X min-1 X g-1 at 60 min of ischemia and in epicardium from 0.27 +/- 0.17 to 0.21 +/- 0.16 ml X min-1 X g-1, both P less than 0.05. In granulocyte-depleted blood-perfused hearts, flow increased over the same period from 0.18 +/- 0.15 to 0.29 +/- 0.18 ml X min-1 X g-1 in endocardium (P less than 0.05) and did not change significantly in epicardium (0.36 +/- 0.22 to 0.41 +/- 0.24 ml X min-1 X g-1). The LEU-depleted blood perfusate contained less than 33 granulocytes/microliter, whereas control perfusate contained 4,265/microliter. Reperfusion at normal pressures with carbon suspension allowed for histologic evaluation of the no-reflow phenomenon. With whole blood perfusion the no-reflow phenomenon in the endocardium was present with 27% of capillaries occluded, compared with nearly complete reperfusion in LEU-depleted animals (1% of capillaries occluded, P less than 0.05). Furthermore, LEU depletion prevented the increases in tissue water content seen in control hearts and decreased the incidence of ventricular arrhythmias. These studies demonstrate the significant participation of granulocytes in the unfavorable responses of flow, edema formation, and arrhythmias to the 1st h of myocardial ischemia and further document their role in the no-reflow phenomenon.
近期证据表明,白细胞(LEU)是大型、僵硬、黏稠的细胞,可自然黏附于血管内皮。白细胞在急性缺血早期心肌微血管反应中的广泛作用体现在以下方面:1)白细胞堵塞毛细血管在无复流现象中的作用;2)输注白细胞后骨骼肌阻力增加;3)抗白细胞药物对缺血心肌的挽救作用。我们在匹配的对照条件下,用全血或去除粒细胞的全血灌注冠状动脉循环。在1小时的缺血期(左前降支闭塞),回旋支灌注压通过伺服控制维持在恒定值。在全血灌注的心脏中,用放射性微球法测得的心内膜血流在缺血5分钟时为0.12±0.05,在缺血60分钟时降至0.09±0.04毫升·分钟⁻¹·克⁻¹;心外膜血流从0.27±0.17降至0.21±0.16毫升·分钟⁻¹·克⁻¹,两者P均小于0.05。在去除粒细胞的血液灌注的心脏中,同期心内膜血流从0.18±0.15增加至0.29±0.18毫升·分钟⁻¹·克⁻¹(P小于0.05),心外膜血流无显著变化(从0.36±0.22至0.41±0.24毫升·分钟⁻¹·克⁻¹)。去除白细胞的血液灌注液中粒细胞含量低于33个/微升,而对照灌注液中粒细胞含量为4265个/微升。用碳混悬液在正常压力下再灌注,以便对无复流现象进行组织学评估。全血灌注时,心内膜出现无复流现象,27%的毛细血管闭塞,而在去除白细胞的动物中几乎完全再灌注(1%的毛细血管闭塞,P小于0.05)。此外,去除白细胞可防止对照心脏中出现的组织含水量增加,并降低室性心律失常的发生率。这些研究表明,粒细胞在心肌缺血第1小时血流、水肿形成和心律失常的不良反应中起重要作用,并进一步证明了它们在无复流现象中的作用。
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