实验性肝硬化并发自发性细菌性腹膜炎:不同治疗方案对内毒素血症和血流动力学紊乱的比较效果

Chinese journal of digestive diseases Pub Date : 2003-07-01 DOI:10.1046/J.1443-9573.2003.T01-1-00122.X

F. Marotta, Y. Naito, A. Helmy, E. Oliva, E. Minelli, M. Yoshioka, C. Min

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After the 6th week of CCL4 administration rats were divided into 5 groups for the remaining 6 weeks: (A) saline b.i.d; (B) lactulose 0.5 g b.i.d.; (C) rifaximine 1 mg b.i.d; (D) 2 mL b.i.d of a probiotic mixture and (E) 1 week of rifaximine followed by 5 weeks of probiotic. \n \n \n \nRESULTS: Rats with cirrhosis and ascites showed a significantly high concentration of either portal, splanchnic and systemic endotoxin, as well as plasma TNF-α concentration (P < 0.05). Rifaximine alone, rifaximine plus probiotic or probiotic alone significantly decreased the plasma endotoxin concentration at each of the three tested sites, as well as the plasma concentration of TNF-α (P < 0.01). Total Gram-negative aerobic bacteria count in the stool markedly decreased together with a significant increase of the enterococcal population in the rifaximine plus probiotic group and, to a lesser extent, in the other treatment groups. 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引用次数: 1

摘要

目的:本研究的目的是从细胞因子级联、内脏和全身血流动力学的角度来评估不同治疗方案在实验性肝硬化中改变肠道微生态的作用。方法:用四氯化碳(CCL4)诱导雄性Sprague-Dawley大鼠肝硬化。CCL4给药第6周后，将大鼠分为5组，其余6周:(A)生理盐水;(B)乳果糖0.5 g b.i.d;(C)利福昔明1mg b.i.d;(D)每日2ml益生菌混合物，(E) 1周利福昔明，随后5周益生菌。结果:肝硬化和腹水大鼠门脉、内脏和全身内毒素浓度及血浆TNF-α浓度均显著升高(P < 0.05)。利福昔明单用、利福昔明联合益生菌或单用益生菌均显著降低3个试验点血浆内毒素浓度和血浆TNF-α浓度(P < 0.01)。在利福昔明加益生菌组中，粪便中革兰氏阴性需氧细菌总数显著减少，肠球菌数量显著增加，其他治疗组的情况则较轻。治疗大鼠细菌性腹膜炎发生率明显降低，利福昔明加益生菌治疗是最有效的方案。每一种治疗方法都显著降低了肠系膜淋巴结或门静脉样本的阳性培养百分比，利福昔明加益生菌是最有效的。与健康对照大鼠相比，肝硬化大鼠的平均动脉压和全身血管阻力明显降低，但心脏指数和门静脉压力较高。自发性细菌性腹膜炎进一步加重了全身血管阻力，但利福昔明加益生菌治疗可部分改善这种情况。结论:这些数据表明，一种不可吸收的抗生素与一种益生菌联合使用，可能通过对内毒素的影响和对TNF - α释放的间接抑制，对严重肝硬化过程中异常的全身血管扩张反应有有益的影响。

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Spontaneous bacterial peritonitis associated with experimental cirrhosis: Comparative effect of different therapeutic options on endotoxinemia and hemodynamic derangement

OBJECTIVE: The aim of this investigation was to assess the role of different therapeutic options aimed at modifying the gut microecology in experimental liver cirrhosis in view of the cytokine cascade and splanchnic and systemic hemodynamics. METHODS: Cirrhosis was induced in male Sprague-Dawley rats by carbon tetrachloride (CCL4). After the 6th week of CCL4 administration rats were divided into 5 groups for the remaining 6 weeks: (A) saline b.i.d; (B) lactulose 0.5 g b.i.d.; (C) rifaximine 1 mg b.i.d; (D) 2 mL b.i.d of a probiotic mixture and (E) 1 week of rifaximine followed by 5 weeks of probiotic. RESULTS: Rats with cirrhosis and ascites showed a significantly high concentration of either portal, splanchnic and systemic endotoxin, as well as plasma TNF-α concentration (P < 0.05). Rifaximine alone, rifaximine plus probiotic or probiotic alone significantly decreased the plasma endotoxin concentration at each of the three tested sites, as well as the plasma concentration of TNF-α (P < 0.01). Total Gram-negative aerobic bacteria count in the stool markedly decreased together with a significant increase of the enterococcal population in the rifaximine plus probiotic group and, to a lesser extent, in the other treatment groups. Treated rats showed a significantly decreased occurrence of bacterial peritonitis and the rifaximine plus probiotic treatment was the most effective regimen. Each of the treatments significantly reduced the percentage of positive culture of either mesenteric lymph node or portal vein samples, rifaximine plus probiotic being the most effective. As compared with healthy control rats, those with cirrhosis showed a significantly lower mean arterial pressure and systemic vascular resistance, but a higher cardiac index and portal pressure. Spontaneous bacterial peritonitis further worsened the systemic vascular resistance, but this was partly improved by the rifaximine plus probiotic treatment. CONCLUSION: These data suggest that the association of a nonabsorbable antibiotic with a probiotic beneficially affects the abnormal systemic vasodilatory response in the course of severe liver cirrhosis, probably through the effects on endotoxin and indirect inhibition of TNF−α release.

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Chinese journal of digestive diseases

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