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首页> 外文期刊>World Journal of Surgery: Official Journal of the Societe Internationale de Chirurgie, Collegium Internationale Chirurgiae Digestivae, and of the International Association of Endocrine Surgeons >Effect of short-term administration of prostaglandin E1 on viability after ischemia/reperfusion injury with extended hepatectomy in cirrhotic rat liver.
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Effect of short-term administration of prostaglandin E1 on viability after ischemia/reperfusion injury with extended hepatectomy in cirrhotic rat liver.

机译:短期给予前列腺素E1对肝硬化大鼠肝脏缺血/再灌注损伤及扩大肝切除术后存活力的影响。

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摘要

The cytoprotective effect of prostaglandin E(1) (PGE(1)) has been demonstrated experimentally and clinically against hepatic ischemia and reperfusion injury and against the effects of partial hepatectomy in both individual and combined models of noncirrhotic livers. Cirrhotic livers are more vulnerable to ischemia/reperfusion injury during hepatectomy than are noncirrhotic livers, and postoperative malfunctioning complicates life with multiple organ failure. Cirrhotic livers with tumors have mostly been treated conservatively because extended hepatectomy with induced ischemia during surgery is impossible. The purpose of our study was to document postoperative surgical adaptation in inoperable cases with improved survival after extended hepatectomy in a rat model of cirrhosis treated by PGE(1). Cirrhosis was induced by intraperitoneal injections of 1% dimethylnitrosamine. The liver was subjected to 15 minutes of total ischemia by occluding the hepatoduodenal ligament. Hepatectomy was performed during ischemia. Pretreatment with PGE(1) (0.4 microg/kg/min) (or without it in the controls) was given for 15 minutes by intravenous infusion prior to inducing ischemia and during reperfusion. Portal venous flow (PVF) and liver tissue blood flow (LTBF) were measured during reperfusion. At the end of 60 minutes of reperfusion, venous blood was collected for liver function tests. The animals were followed up regarding survival for 48 hours. The PVF and LTBF were significantly improved in the PGE(1) group. The blood chemical analysis indicated that PGE(1) significantly suppressed posthepatectomy liver dysfunction. Most importantly, PGE(1) treatment markedly improved the survival rate, from 42% in the controls to 75% in the test animals at 24 hours after hepatectomy and from 17% in the controls to 58% in the test animals at 48 hours. We concluded that short-term administration of PGE(1) makes extensive hepatectomy possible under ischemic conditions in cirrhotic livers.
机译:前列腺素E(1)(PGE(1))的细胞保护作用已在实验和临床上证明了在非肝硬化肝的个体模型和联合模型中对肝脏缺血和再灌注损伤以及部分肝切除的作用。与非肝硬化肝相比,肝硬化肝较非肝硬化肝更容易遭受缺血/再灌注损伤,并且术后功能异常使生命复杂化,并伴有多器官衰竭。肝硬化伴肿瘤的肝癌大多已被保守治疗,因为不可能在手术期间进行扩大的肝切除术并诱发局部缺血。我们的研究目的是记录在用PGE(1)治疗的肝硬化大鼠模型中,扩大肝切除术后无法手术并具有更好生存率的术后手术适应性。腹膜内注射1%二甲基亚硝胺可诱发肝硬化。通过闭塞肝十二指肠韧带使肝脏经受总缺血15分钟。缺血期间进行肝切除术。在诱发缺血之前和再灌注期间,通过静脉输注给予PGE(1)(0.4 microg / kg / min)(或在对照组中不使用)进行15分钟的预处理。在再灌注期间测量门静脉血流(PVF)和肝组织血流(LTBF)。再灌注60分钟后,收集静脉血进行肝功能检查。对动物进行关于存活48小时的随访。 PGE(1)组的PVF和LTBF明显改善。血液化学分析表明,PGE(1)显着抑制了肝切除术后肝功能障碍。最重要的是,PGE(1)治疗显着提高了存活率,从肝切除术后24小时的对照组动物的存活率提高到了42%,而在48小时时的对照组动物的存活率则从17%提高到58%。我们得出的结论是,在缺血性肝硬化肝脏中,短期给予PGE(1)可以使广泛的肝切除成为可能。

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