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肝性脑病的药物治疗。

Pharmacotherapy for hepatic encephalopathy.

机构信息

Department of Clinical Pharmacy, University of Southern California School of Pharmacy, USC University Hospital Department of Pharmacy, Los Angeles, California, USA.

出版信息

Drugs. 2010 Jun 18;70(9):1131-48. doi: 10.2165/10898630-000000000-00000.

Abstract

Hepatic encephalopathy (HE) is a challenging clinical complication of liver dysfunction with a wide spectrum of neuropsychiatric abnormalities that range from mild disturbances in cognitive function and consciousness to coma and death. The pathogenesis of HE in cirrhosis is complex and multifactorial, but a key role is thought to be played by circulating gut-derived toxins of the nitrogenous compounds, most notably ammonia. Therapeutic treatment options for HE are currently limited and have appreciable risks and benefits associated with their use. Management of HE primarily involves avoidance of precipitating factors, limitation of dietary protein intake, and administration of various ammonia-lowering therapies such as non-absorbable disaccharides and select antimicrobial agents. Non-absorbable disaccharides, such as lactulose, have traditionally been regarded as first-line pharmacotherapy for patients with HE. However, multiple adverse events have been associated with their use. In addition, recent literature has questioned the true efficacy of the disaccharides for this indication. Neomycin, metronidazole and vancomycin may be used as alternative treatments for patients intolerant or unresponsive to non-absorbable disaccharides. Antimicrobials reduce bacterial production of ammonia and other bacteria-derived toxins through suppression of intestinal flora. Neomycin has been reported to be as effective as lactulose, and similar efficacy has been reported with vancomycin and metronidazole for the management of HE. However, the adverse effects frequently associated with these antimicrobials limit their use as first-line pharmacological agents. Neomycin is the most commonly used antimicrobial for HE and, although poorly absorbed, systemic exposure to the drug in sufficient amounts causes hearing loss and renal toxicity. Long-term neomycin therapy requires annual auditory testing and continuous monitoring of renal function. Long-term use of metronidazole has been associated with neurotoxicity in patients with cirrhosis, including dose-dependent peripheral neuropathy. Vancomycin may be a safer option for HE in patients with chronic liver disease; however, limited experience, possible bacterial overgrowth and risk for enteric bacteria resistance preclude the routine use of vancomycin for HE. Rifaximin is a novel antimicrobial agent with a wide spectrum of activity that has shown promise as an alternative antimicrobial treatment option for HE. Several clinical trials have compared rifaximin to the disaccharides, lactulose and lactitol, and the antimicrobial neomycin. Rifaximin appears to be at least as effective as conventional drug therapy and has been associated with fewer adverse effects due to its limited systemic absorption. The available clinical data appear to support a favourable benefit-risk ratio for rifaximin, which has shown efficacy with an improved tolerability profile. Future studies are needed in order to truly characterize its cost effectiveness in today's healthcare environment. Other less frequently utilized alternative treatment options include administration of benzodiazepine receptor antagonists, branched-chain amino acids, ornithine aspartate, zinc supplementation, sodium benzoate, dopamine receptor agonists, acarbose and probiotics. Presently, there is relatively limited clinical data supporting their routine use in HE.

摘要

肝性脑病 (HE) 是一种具有广泛神经精神异常的肝功能障碍的挑战性临床并发症,从轻度认知功能和意识障碍到昏迷和死亡不等。肝硬化 HE 的发病机制复杂且多因素,但循环肠道来源的含氮化合物毒素被认为是一个关键因素,其中最重要的是氨。目前,HE 的治疗方法选择有限,并且与使用相关联具有显著的风险和益处。HE 的主要治疗方法包括避免诱发因素、限制饮食蛋白摄入以及使用各种降低氨的治疗方法,如非吸收性双糖和选择性抗菌药物。非吸收性双糖,如乳果糖,传统上被认为是 HE 患者的一线药物治疗方法。然而,其使用与多种不良反应相关。此外,最近的文献质疑双糖在该适应证中的真正疗效。新霉素、甲硝唑和万古霉素可作为不耐受或对非吸收性双糖无反应的患者的替代治疗方法。抗菌药物通过抑制肠道菌群减少细菌产生的氨和其他细菌来源的毒素。据报道,新霉素与乳果糖一样有效,并且万古霉素和甲硝唑在管理 HE 方面也有类似的疗效。然而,这些抗菌药物经常出现的不良反应限制了它们作为一线药物的使用。新霉素是最常用于治疗 HE 的抗菌药物,尽管吸收不良,但药物在足够量时全身暴露会导致听力损失和肾毒性。长期新霉素治疗需要每年进行听觉测试和连续监测肾功能。长期使用甲硝唑与肝硬化患者的神经毒性有关,包括剂量依赖性周围神经病。万古霉素可能是慢性肝病患者 HE 的更安全选择;然而,有限的经验、可能的细菌过度生长和肠道细菌耐药性的风险排除了万古霉素常规用于 HE。利福昔明是一种具有广泛活性的新型抗菌药物,作为 HE 的替代抗菌治疗选择具有前景。几项临床试验将利福昔明与双糖、乳果糖和乳糖醇以及抗菌药物新霉素进行了比较。利福昔明似乎至少与常规药物治疗一样有效,并且由于其有限的全身吸收,与不良反应相关较少。现有的临床数据似乎支持利福昔明的有利风险效益比,其具有改善的耐受性特征。为了真正确定其在当今医疗保健环境中的成本效益,需要进行进一步的研究。其他不太常用的替代治疗方法包括苯二氮䓬受体拮抗剂、支链氨基酸、天冬氨酸鸟氨酸、锌补充剂、苯甲酸钠、多巴胺受体激动剂、阿卡波糖和益生菌的使用。目前,支持其在 HE 中常规使用的临床数据相对有限。

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