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A new macrocyclic antibiotic, fidaxomicin (OPT-80), causes less alteration to the bowel microbiota of Clostridium difficile-infected patients than does vancomycin

机译:一种新的大环抗生素,Fidaxomicin(OPT-80),对梭菌感染患者的肠道微生物群较少,而不是万古霉素

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Clostridium difficile infection (CDI) is the most common identifiable cause of diarrhoea in hospitalized patients. Current therapies rely on the administration of metronidazole or vancomycin, which reduce vegetative populations of C. difficile in the bowel. Recurrence of the disease when treatment with these antibiotics ceases indicates that metronidazole and vancomycin affect not only C. difficile but also commensal populations that normally mediate competitive exclusion. Fidaxomicin is a new antibiotic that inhibits C. difficile. Our study shows that fidaxomicin had little effect on the composition of the faecal microbiota in terms of its major phylogenetic clusters. Notably, clostridial clusters XIVa and IV, and Bifidobacterium, were much less affected by fidaxomicin compared to vancomycin treatment. These findings help to explain the substantially reduced rates of relapse following treatment of CDI with fidaxomicin in recent clinical trials.
机译:Clostridium Interscile感染(CDI)是住院患者中最常见的腹泻的可识别原因。目前的疗法依赖于甲硝唑或万古霉素的施用,从而减少了肠道中C.艰难梭菌的营养群。使用这些抗生素治疗时疾病的复发表明甲硝唑和万古霉素不仅影响艰难梭菌,而且影响通常介导竞争排斥的共生群体。 Fidaxomicin是一种抑制C.艰难术的新抗生素。我们的研究表明,Fidaxomicin在其主要系统发育簇方面对粪便微生物群的组成几乎没有影响。值得注意的是,与万象素治疗相比,梭菌簇Xiva和IV和双歧杆菌受到百分比细胞的影响要小得多。这些发现有助于解释在最近的临床试验中治疗Fidaxomicin的CDI后显着降低的复发率。

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