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IntraportalversusSystemic Pentoxifylline Infusion after Normothermic Liver Ischemia: Effects on Regional Blood Flow Redistribution and Hepatic Ischemia-Reperfusion Injury

机译:正常体温肝脏缺血后门静脉输注全身性己酮可可碱的输注:对区域血流再分配和肝缺血-再灌注损伤的影响

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Pentoxifylline (PTX) has been shown to have beneficial effects on microcirculatory blood flow. In this study we evaluate the potential hemodynamic and metabolic benefits of PTX during hepatic ischemia. We also test the hypothesis that portal PTX infusion can minimize the I/R injury when compared to systemic infusion.Methods. Twenty-four dogs (18.1±0.7 kg) were subjected to portal triad occlusion (PTO) for 45 min. The animals were assigned to 3 groups: CT (control, PTO,n=8), PTX-syst (PTO + 25 mg/Kg of PTX IV,n=8), and PTX-pv (PTO + 25 mg/Kg of PTX in the portal vein,n=8). Animals were followed for 120 min. Systemic hemodynamics, gastrointestinal tract perfusion, oxygen-derived variables, and liver enzymes were evaluated throughout the experiment.Results.Animals treated with PTX presented significantly higher CO in the first hour after reperfusion, when compared to the CT (~3.7 vs. 2.1 L/min,P<0.05). Alanine aminotransferase (ALT) was similar in the PTX groups two hours after reperfusion but significantly higher in the CT (227 vs.~64 U/L,P<0.05).Conclusion. PTX infusion was associated with hemodynamic benefits and was able to minimize liver injury during normothermic hepatic I/R. However, local PTX infusion was not associated with any significant advantage over systemic route.
机译:己酮可可碱(PTX)已显示对微循环血流具有有益作用。在这项研究中,我们评估了肝缺血期间PTX的潜在血流动力学和代谢益处。我们还检验了以下假设:与全身输注相比,门脉PTX输注可以最大程度地减少I / R损伤。对二十四只狗(18.1±0.7 kg)进行门禁三联征(PTO)45min。将动物分为三组:CT(对照组,PTO,n = 8),PTX-syst(PTO +25μmg/ Kg PTX IV,n = 8)和PTX-pv(PTO +25μmg/ Kg PTX)。门静脉PTX,n = 8)。跟踪动物120分钟。在整个实验过程中评估了全身血流动力学,胃肠道灌注,氧衍生变量和肝酶结果。与CT相比,PTX处理的​​动物在再灌注后的第一小时内CO显着升高(〜3.7 vs 2.1 L /min,P<0.05)。再灌注后两小时PTX组丙氨酸转氨酶(ALT)相似,但CT显着升高(227 vs.〜64 U / L,P <0.05)。 PTX输注与血液动力学益处相关,并且能够使常温肝I / R期间的肝损伤最小化。但是,局部PTX输注与全身性输注相比无明显优势。

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