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肝素涂层体外循环中的高剂量与低剂量肝素:补体和粒细胞的激活

High and low heparin dose with heparin-coated cardiopulmonary bypass: activation of complement and granulocytes.

作者信息

Ovrum E, Mollnes T E, Fosse E, Holen E A, Tangen G, Ringdal M A, Videm V

机构信息

Department of Cardiac Surgery and Anesthesiology, Oslo Heart Center, Norway.

出版信息

Ann Thorac Surg. 1995 Dec;60(6):1755-61. doi: 10.1016/0003-4975(95)00763-6.

Abstract

BACKGROUND

Cardiopulmonary bypass with heparin-coated circuits allows reduced amounts of systemic heparin. Heparin inhibits activation of the complement cascade experimentally, but the effects of different levels of systemic heparin on activation of complement and granulocytes in patients have remained unknown.

METHODS

Fifty-two patients undergoing coronary artery bypass procedures were studied. Cardiopulmonary bypass circuits completely coated with surface-bound heparin were used for one group given low-dose heparin (n = 17) (activated clotting time > 250 seconds), and was compared with a second group having normal high-dose heparin (activated clotting time > 480 seconds) (n = 18). A third control group was perfused with ordinary uncoated circuits and a full heparin dose (n = 17).

RESULTS

During cardiopulmonary bypass, the C3 activation products C3b, iC3b, and C3c increased markedly in all three groups compared with baseline, but significantly less in the two heparin-coated groups (high dose, median maximal increase 58 arbitrary units (AU)/mL; low dose, 48 AU/mL) compared with the uncoated control group (74 AU/mL) (p < 0.01). The difference between the two coated groups was not significant. Similarly, the maximal increase in terminal SC5b-9 complement complex was considerably lower in the heparin-coated groups (high dose, 2.5 AU/mL; low dose, 2.6 AU/mL) compared with the level observed in the uncoated control group (5.3 AU/mL) (p < 0.01). The release of the granulocyte activation enzymes myeloperoxidase and lactoferrin increased from the beginning of the operation, with peak levels at the end of cardiopulmonary bypass (p < 0.01). The concentration of lactoferrin was significantly (p < 0.01) reduced in the low heparin dose group compared with the two other groups receiving normal high heparin doses, indicating that circulating heparin is an important granulocyte agonist, acting independently of the presence or absence of heparin-coated surfaces. Also for myeloperoxidase a higher level was observed in the high heparin dose group.

CONCLUSIONS

Complement activation was significantly reduced in both heparin-coated groups and was independent of the level of systemic heparinization, whereas granulocyte activation was reduced only in patients who received low doses of systemically administered heparin. The results indicate that a moderate reduction of the systemic heparin dose may be an advantage with regard to improved biocompatibility when using heparin-coated cardiopulmonary bypass circuits.

摘要

背景

使用肝素涂层回路进行体外循环可减少全身肝素用量。实验表明肝素可抑制补体级联反应的激活,但不同水平的全身肝素对患者补体和粒细胞激活的影响尚不清楚。

方法

对52例行冠状动脉搭桥手术的患者进行研究。一组(n = 17)使用完全涂有表面结合肝素的体外循环回路并给予低剂量肝素(活化凝血时间> 250秒),并与另一组给予正常高剂量肝素(活化凝血时间> 480秒)(n = 18)进行比较。第三对照组使用普通未涂层回路和全剂量肝素进行灌注(n = 17)。

结果

在体外循环期间,与基线相比,所有三组中C3激活产物C3b、iC3b和C3c均显著增加,但与未涂层对照组(74任意单位(AU)/ mL)相比,两个肝素涂层组(高剂量,最大增加中位数58 AU / mL;低剂量,48 AU / mL)增加明显较少(p < 0.01)。两个涂层组之间的差异不显著。同样,与未涂层对照组(5.3 AU / mL)相比,肝素涂层组中末端SC5b-9补体复合物的最大增加量也显著降低(高剂量,2.5 AU / mL;低剂量,2.6 AU / mL)(p < 0.01)。粒细胞激活酶髓过氧化物酶和乳铁蛋白的释放从手术开始时就增加,在体外循环结束时达到峰值水平(p < 0.01)。与接受正常高剂量肝素的其他两组相比,低肝素剂量组中乳铁蛋白的浓度显著降低(p < 0.01),表明循环肝素是一种重要的粒细胞激动剂,其作用与肝素涂层表面的有无无关。对于髓过氧化物酶,高肝素剂量组中也观察到较高水平。

结论

两个肝素涂层组中的补体激活均显著降低,且与全身肝素化水平无关,而粒细胞激活仅在接受低剂量全身肝素治疗的患者中降低。结果表明,在使用肝素涂层体外循环回路时,适度降低全身肝素剂量可能有利于改善生物相容性。

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