血液冬眠：一种抑制心肺转流引起的全身炎症和凝血的新策略。

Blood hibernation: a novel strategy to inhibit systemic inflammation and coagulation induced by cardiopulmonary bypass.

机构信息

Laboratory Medicine, West China Hospital, Sichuan University, Chengdu, Sichuan 610041, China.

出版信息

Chin Med J (Engl). 2010 Jul;123(13):1741-7.

PMID:20819640

Abstract

BACKGROUND

Inflammation and coagulation are two intimately cross-linked defense mechanisms of most, if not all organisms to injuries. During cardiopulmonary bypass (CPB), these two processes are activated and interact with each other through several common pathways, which may result in subsequent organ dysfunction. In the present study, we hypothesized that the addition of nitric oxide, prostaglandin E1 (PGE1), and aprotinin to the systemic circulation, hereby referred to as blood hibernation, would attenuate the inflammation and coagulation induced by CPB.

METHODS

Thirty adult mongrel dogs were equally divided into five groups, anesthetized and placed on hypothermic CPB (32 degrees C). Each group received respectively the following treatments: (1) inhalation of 40 ppm nitric oxide; (2) intravenous infusion of 20 ng x kg(-1) x min(-1) of PGE1; (3) 80,000 kallikrein inhibitor units (KIU)/kg of aprotinin; (4) the combination of all three agents (blood hibernation group); and (5) no treatment (control group) during CPB. Activation of leukocyte, platelet, endothelial cell, and formation of thrombin were assessed after CPB.

RESULTS

As compared with the other four groups, leukocyte counts were higher, while plasma elastase, interleukin-8, CD11b mRNA expression, myeloperoxidase activities and lung tissue leukocyte counts were lower in the blood hibernation group (P < 0.05 versus other four groups after CPB). Plasma prothrombin fragment (PTF)1+2, and platelet activation factors were lower, while platelet counts were higher in the blood hibernation group (P < 0.05 versus other four groups at 6 and 12 hours after CPB). Electron microscopy showed endothelial pseudopods protrusion, with cell adherence in all four groups except the blood hibernation group where endothelial cells remained intact.

CONCLUSION

Blood hibernation, effected by the addition of nitric oxide, PGE1 and aprotinin to the circulating blood during extra-corporeal circulation, was observed to attenuate the inflammation and coagulation induced by cardiopulmonary bypass, most likely by inhibiting the important common intermediates between the two cross-linked processes.

摘要

背景

炎症和凝血是大多数（如果不是全部）生物体对损伤的两种密切相关的防御机制。在体外循环（CPB）期间，这两个过程被激活并通过几个共同途径相互作用，这可能导致随后的器官功能障碍。在本研究中，我们假设将一氧化氮、前列腺素 E1（PGE1）和抑肽酶添加到体循环中，即血液冬眠，将减轻 CPB 引起的炎症和凝血。

方法

30 只成年杂种狗被平均分为五组，麻醉并置于低温 CPB（32°C）下。每组分别接受以下治疗：（1）吸入 40 ppm 一氧化氮；（2）静脉输注 20 ng·kg-1·min-1 的 PGE1；（3）80000 单位/kg 的抑肽酶；（4）所有三种药物的组合（血液冬眠组）；（5）CPB 期间不治疗（对照组）。CPB 后评估白细胞、血小板、内皮细胞的激活和凝血酶的形成。

结果

与其他四组相比，血液冬眠组白细胞计数较高，而血浆弹性蛋白酶、白细胞介素-8、CD11b mRNA 表达、髓过氧化物酶活性和肺组织白细胞计数较低（CPB 后与其他四组相比，P<0.05）。血液冬眠组血浆凝血酶原片段（PTF）1+2 和血小板激活因子较低，血小板计数较高（CPB 后 6 和 12 小时与其他四组相比，P<0.05）。电镜显示内皮伪足突出，除血液冬眠组外，所有四组均有细胞黏附，而血液冬眠组内皮细胞保持完整。