首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >Attenuation of tissue thrombosis and hemorrhage by ala-TFPI does not account for its protection against E. coli--a comparative study of treated and untreated non-surviving baboons challenged with LD100 E. coli.
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Attenuation of tissue thrombosis and hemorrhage by ala-TFPI does not account for its protection against E. coli--a comparative study of treated and untreated non-surviving baboons challenged with LD100 E. coli.

机译:ala-TFPI减轻组织血栓形成和出血并不能说明其对大肠杆菌的保护作用-一项针对经过处理和未经处理的,受到LD100大肠杆菌攻击的非存活狒狒的比较研究。

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This study was designed to determine the effect of a delayed infusion (T+120 min) of alanyl tissue factor pathway inhibitor (ala-TFPI) on the response to LD100 E. coli. We hypothesized that baboons treated with a low dose of TFPI (5 mg/kg) which did not survive would exhibit thrombosis, infarction and hemorrhage of target tissues such as that seen in untreated animals infused with LD100 E. coli. Eight baboons were infused with 5 mg/kg of ala-TFPI over a 10 h period beginning immediately after a 2 h infusion of LD100 E. coli (experimental group). Four baboons were infused with E. coli followed by a 10 h infusion of saline (control group). Of the 12 baboons, the 11 non-survivors (TFPI = 7 out of 8; controls = 4 out of 4) were evaluated for the extent of thrombosis, necrosis, hemorrhage, and congestion of target tissues and for changes in clinical chemical parameters. We expected that failure to protect would correlate with failure to inhibit thrombosis of target tissue (8). Surprisingly ala-TFPI significantly inhibited thrombosis, hemorrhage and necrosis of adrenal and renal tissues and attenuated the rise in creatinine in the 7 treated non-survivors. The lungs of these non-survivors, however, exhibited intra-alveolar fibrin and a mild degree of hemorrhage and edema. We concluded that low doses of ala-TFPI begun as late as T+120 in minutes failed to protect against the lethal effects of LD100 E. coli in spite of completely preventing thrombosis and hemorrhage in target organs, and that thrombosis, infarction and hemorrhage of adrenal and renal tissue are not part of the lethal chain of events in this IV model of E. coli sepsis.
机译:这项研究的目的是确定延迟输注(T + 120分钟)丙氨酰组织因子途径抑制剂(ala-TFPI)对LD100大肠杆菌反应的影响。我们假设用低剂量的TFPI(5 mg / kg)处理过的狒狒无法存活,它们会表现出目标组织的血栓形成,梗塞和出血,例如在未注射LD100大肠杆菌的动物中所见。在LD100大肠杆菌2小时的注入后的10小时内,八个狒狒被注入了5 mg / kg的ala-TFPI(实验组)。向四个狒狒注入大肠杆菌,然后注入盐水10 h(对照组)。在12只狒狒中,评估了11名非幸存者(TFPI = 8分之7;对照组= 4分之4)对目标组织的血栓形成,坏死,出血和充血程度以及临床化学参数的变化。我们预计,保护失败将与抑制靶组织血栓形成相关(8)。出乎意料的是,ala-TFPI可以显着抑制肾上腺和肾脏组织的血栓形成,出血和坏死,并减弱了7个未经治疗的幸存者中肌酐的升高。然而,这些非幸存者的肺部表现为肺泡内纤维蛋白和轻度的出血和水肿。我们得出的结论是,尽管完全预防了靶器官的血栓形成和出血,并且低剂量的ala-TFPI甚至在T + 120几分钟之内就开始未能预防LD100大肠杆菌的致死作用,并且仍无法预防LD100大肠杆菌的致死作用。在该大肠杆菌败血症的IV模型中,肾上腺和肾组织不是致命的事件链的一部分。

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