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Short-course therapy for diarrhea-predominant irritable bowel syndrome: understanding the mechanism impact on gut microbiota and safety and tolerability of rifaximin

机译:腹泻型肠易激综合征的短程治疗:了解利福昔明的作用机理对肠道菌群的影响以及利福昔明的安全性和耐受性

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摘要

Irritable bowel syndrome (IBS) is a common gastrointestinal (GI) disorder characterized by abdominal pain that occurs with defecation or alterations in bowel habits. Further classification is based on the predominant bowel habit: constipation-predominant IBS, diarrhea-predominant IBS (IBS-D), or mixed IBS. The pathogenesis of IBS is unclear and is considered multifactorial in nature. GI dysbiosis, thought to play a role in IBS pathophysiology, has been observed in patients with IBS. Alterations in the gut microbiota are observed in patients with small intestinal bacterial overgrowth, and overgrowth may occur in a subset of patients with IBS. The management of IBS includes therapies targeting the putative factors involved in the pathogenesis of the condition. However, many of these interventions (eg, eluxadoline and alosetron) require long-term, daily administration and have important safety considerations. Agents thought to modulate the gut microbiota (eg, antibiotics and probiotics) have shown potential benefits in clinical studies. However, conventional antibiotics (eg, neomycin) are associated with several adverse events and/or the risk of bacterial antibiotic resistance, and probiotics lack uniformity in composition and consistency of response in patients. Rifaximin, a nonsystemic antibiotic administered as a 2-week course of therapy, has been shown to be safe and efficacious for the treatment of IBS-D. Rifaximin exhibits a favorable benefit-to-harm ratio when compared with daily therapies for IBS-D (eg, alosetron and tricyclic antidepressants), and rifaximin was not associated with the emergence of bacterial antibiotic resistance. Thus, short-course therapy with rifaximin is an appropriate treatment option for IBS-D.
机译:肠易激综合症(IBS)是一种常见的胃肠道(GI)疾病,其特征是排便或排便习惯改变引起的腹痛。根据主要的排便习惯进行进一步分类:以便秘为主的IBS,以腹泻为主的IBS(IBS-D)或混合性IBS。 IBS的发病机制尚不清楚,本质上被认为是多因素的。在IBS患者中已观察到胃肠道异位症,据认为在IBS的病理生理中起作用。在小肠细菌过度生长的患者中观察到肠道菌群的改变,并且过度生长可能发生在一部分IBS患者中。 IBS的治疗包括针对病情发病机制中假定因素的疗法。但是,许多此类干预措施(例如,依拉西多林和阿洛司琼)都需要长期每天进行给药,并具有重要的安全考虑。被认为可调节肠道菌群的药物(例如抗生素和益生菌)已在临床研究中显示出潜在的益处。然而,常规抗生素(例如新霉素)与几种不良事件和/或细菌抗生素抗性的风险有关,并且益生菌在患者中缺乏组成上的一致性和反应的一致性。利福昔明是一种非全身性抗生素,为期2周的疗程,已被证明对IBS-D的治疗安全有效。利福昔明与IBS-D的每日疗法(例如阿洛司琼和三环抗抑郁药)相比,具有有利的利弊比,而利福昔明与细菌耐药性的出现无关。因此,利福昔明的短程治疗是IBS-D的合适治疗选择。

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