Evaluation of rifaximin, placebo and lactulose in reducing the levels of benzodiazepine-like compounds in patients with liver cirrhosis: a pilot study.

I Venturini, A Ferrieri, F Farina, F Cosenza, R Avallone, L Corsi, M Baraldi, M L Zeneroli
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Abstract

Benzodiazepine-like compounds (BZDs), either taken with the diet or synthesized by intestinal bacterial flora, may represent a precipitating factor for hepatic encephalopathy (HE) in cirrhotic patients. We evaluated whether a diet and/or treatment with rifaximin or lactulose can reduce serum concentrations of BZDs in 18 cirrhotic patients without HE. Patients were given a standard diet for 7 days to keep the dietary intake of BZDs constant and were then randomized to a 7-day treatment with rifaximin 1,200 mg/day, lactulose 10-20 g three times daily, or placebo. Blood samples were collected at enrollment, at the end of the diet and drug treatment periods, and 7 days after the drug was stopped (follow-up). Serum concentrations of BZDs were measured by a radioligand binding technique after high-performance liquid chromatography extraction and purification and were expressed as diazepam equivalents (DE). No change in serum BZD concentrations was observed during the diet, while a statistically significant decrease from 105.6 +/- 66.5 to 63.5 +/- 49.5 pmol DE/ml was achieved in rifaximin-treated patients (p < 0.05) but not in patients treated with lactulose or placebo. During the followup, serum BZD concentrations returned to 104.5 +/- 74.0 pmol DE/ml in rifaximin-treated patients (p < 0.05 vs. end-treatment values), while no significant change was observed in the lactulose- and placebo-treated patients. These data indicate that control of bacterial flora with cyclic administration of rifaximin plays a pivotal role in avoiding increased plasma concentrations of BZDs, which represent a precipitating factor for HE inpatients with severe liver disease.

评价利福昔明、安慰剂和乳果糖降低肝硬化患者苯二氮卓类化合物水平:一项初步研究
苯二氮卓类化合物(BZDs),无论是与饮食一起服用还是由肠道菌群合成,都可能是肝硬化患者肝性脑病(HE)的一个诱发因素。我们评估了饮食和/或利福昔明或乳果糖治疗是否可以降低18例无HE肝硬化患者的血清BZDs浓度。患者给予标准饮食7天,以保持BZDs的饮食摄入量不变,然后随机分为7天治疗组:利福昔明1200毫克/天,乳果糖10-20克,每日3次,或安慰剂。在入组时、饮食和药物治疗期结束时和停药后7天(随访)采集血样。经高效液相色谱提取纯化后,采用放射配体结合技术测定BZDs的血清浓度,并以地西泮当量(DE)表示。在饮食过程中,血清BZD浓度没有变化,而利福昔明治疗的患者从105.6 +/- 66.5降至63.5 +/- 49.5 pmol DE/ml (p < 0.05),而乳果糖或安慰剂治疗的患者则没有变化。在随访期间,利福昔明组患者血清BZD浓度恢复到104.5 +/- 74.0 pmol DE/ml(与治疗结束值相比p < 0.05),而乳果糖组和安慰剂组患者无显著变化。这些数据表明,通过循环给药利福昔明控制细菌菌群在避免BZDs血浆浓度升高中起关键作用,BZDs是HE住院患者合并严重肝病的一个诱发因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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