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急性肾衰竭与脓毒症:治疗方法

Acute renal failure and sepsis: therapeutic approaches.

作者信息

Cumming A D

机构信息

University Dept of Medicine, Royal Infirmary, Edinburgh, UK.

出版信息

Nephrol Dial Transplant. 1994;9 Suppl 4:159-63.

PMID:7528364
Abstract

Previous studies of experimental sepsis suggested that excessive systemic vasodilatation might be the stimulus to renal hypofiltration and fluid retention in sepsis. Successful therapy for this syndrome requires agents that either act to improve systemic haemodynamics without adverse renal effects, or that act directly on the kidney without impairing circulatory homeostasis. The plasma kallikrein-kinin system is a potent vasodilator pathway, activated by endotoxin. We studied the effect of aprotinin (Trasylol), which inhibits plasma kallikrein, in an ovine model of surgically-induced intra-abdominal sepsis. Given either as an early or late intervention, aprotinin was associated with increased mean arterial pressure and systemic vascular resistance, improved glomerular filtration rate, and increased urinary sodium excretion. In further studies, treatment with the thromboxane synthetase inhibitor, U63,557A (Upjohn), either before or after the surgical induction of peritonitis, was associated with increased glomerular filtration rate and sodium excretion, without any effect on systemic haemodynamics. Logical use of specific antagonists, based on an understanding of the pathophysiology of the septic ARF syndrome, is a desirable strategy.

摘要

以往对实验性脓毒症的研究表明,全身性血管过度扩张可能是脓毒症时肾滤过减少和液体潴留的刺激因素。针对该综合征的成功治疗需要使用既能改善全身血流动力学又无不良肾脏影响的药物,或者直接作用于肾脏而不损害循环稳态的药物。血浆激肽释放酶-激肽系统是一条由内毒素激活的强大血管舒张途径。我们在绵羊手术诱导的腹腔内脓毒症模型中研究了抑制血浆激肽释放酶的抑肽酶(Trasylol)的作用。抑肽酶无论是早期还是晚期干预给药,均与平均动脉压升高、全身血管阻力增加、肾小球滤过率改善以及尿钠排泄增加有关。在进一步的研究中,在手术诱导腹膜炎之前或之后使用血栓素合成酶抑制剂U63,557A(Upjohn)进行治疗,与肾小球滤过率和钠排泄增加有关,而对全身血流动力学没有任何影响。基于对脓毒症性急性肾衰竭综合征病理生理学的理解,合理使用特异性拮抗剂是一种理想的策略。

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