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体外循环期间的低温会延迟但不会阻止中性粒细胞与内皮细胞的黏附。一项临床研究。

Hypothermia during cardiopulmonary bypass delays but does not prevent neutrophil-endothelial cell adhesion. A clinical study.

作者信息

Le Deist F, Menasché P, Kucharski C, Bel A, Piwnica A, Bloch G

机构信息

Department of Cardiovascular Surgery, H pital Lariboisière, France.

出版信息

Circulation. 1995 Nov 1;92(9 Suppl):II354-8. doi: 10.1161/01.cir.92.9.354.

Abstract

BACKGROUND

An accurate evaluation of warm heart surgery cannot be limited to the assessment of the myocardial effects of warm blood cardioplegia but should also address the effects of systemic normothermia on the inflammatory response to cardiopulmonary bypass. A major component of this response is the endothelial adhesion of neutrophils, because it is linked to the release of cytotoxic compounds. This study was designed (1) to characterize the bypass-induced changes in the expression of neutrophil adhesion molecules (L-selectin and beta 2-integrins) and (2) to assess the influence of bypass temperature on these changes.

METHODS AND RESULTS

Twenty case-matched patients undergoing open-heart procedures were divided into two equal groups according to the core temperature during cardiopulmonary bypass: warm (33.4 +/- 0.3 degrees C) or cold (27.1 +/- 0.4 degrees C, P < .0001 versus warm). Arterial blood samples were collected before, during, and 30 minutes after bypass and processed for the expression of L-selectin and beta 2-integrins (CD11a, CD11b, and CD11c) with flow cytometry. Warm bypass was associated with an early and sustained upregulation of CD11b. In contrast, hypothermia resulted in a strikingly less pronounced CD11b upregulation during bypass. However, CD11b expression sharply increased thereafter so that 30 minutes after bypass, it was no longer significantly different between the two groups. Changes in CD11c expression grossly paralleled those described for CD11b. Neither CD11a nor L-selectin changed significantly from baseline values in either group.

CONCLUSIONS

Clinical cardiopulmonary bypass is associated with a marked upregulation of the neutrophil CD11b and CD11c integrins. Hypothermia delays but does not prevent the increased expression of these adhesion molecules, which could consequently represent logical targets for interventions designed to blunt the neutrophil-mediated component of bypass-induced inflammatory tissue damage.

摘要

背景

对心脏温血手术的准确评估不能仅限于评估温血心脏停搏液对心肌的影响,还应考虑全身正常体温对体外循环炎症反应的影响。这种反应的一个主要成分是中性粒细胞的内皮黏附,因为它与细胞毒性化合物的释放有关。本研究旨在(1)描述体外循环引起的中性粒细胞黏附分子(L-选择素和β2整合素)表达变化,以及(2)评估体外循环温度对这些变化的影响。

方法与结果

20例接受心脏直视手术的病例匹配患者,根据体外循环期间的核心温度分为两组,每组人数相等:温血组(33.4±0.3℃)和冷血组(27.1±0.4℃,与温血组相比P<0.0001)。在体外循环前、期间和结束后30分钟采集动脉血样本,用流式细胞术检测L-选择素和β2整合素(CD11a、CD11b和CD11c)的表达。温血体外循环与CD11b的早期持续上调有关。相比之下,低温导致体外循环期间CD11b上调明显不明显。然而,此后CD11b表达急剧增加,因此在体外循环后30分钟,两组之间不再有显著差异。CD11c表达的变化与CD11b的变化大致平行。两组中CD11a和L-选择素均未与基线值发生显著变化。

结论

临床体外循环与中性粒细胞CD11b和CD11c整合素的显著上调有关。低温延迟但不能阻止这些黏附分子表达的增加,因此这些黏附分子可能是旨在减轻体外循环引起的炎症组织损伤中中性粒细胞介导成分的干预措施的合理靶点。

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