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The Possible Innovative Use of Bifidobacterium longum W11 in Association With Rifaximin: A New Horizon for Combined Approach?

机译:长双歧杆菌W11与利福昔明联合使用的可能创新用途:联合治疗的新视野?

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Goals:The aim of the study was to unequivocally demonstrate the nontransmissibility of the genes mediating the resistance of the strain Bifidobacterium longum W11 (LMG P-21586) to rifaximin.Background:Most antibiotic treatments can induce unfavorable side effects such as antibiotic-associated diarrhea, which is largely attributable to the disruption of the intestinal microbiota. The parallel intake of probiotic bacteria might reduce these events, even if with generally very poor results. In this regard, the use of antibiotic-resistant beneficial bacteria could represent a worthy strategy.Study:Rifaximin was tested in parallel with rifampicin, rifapentine, and rifabutin, all rifamycin derivates, using 5 different concentrations. Susceptibility tests were performed by the disc diffusion method of Kirby-Bauer, and inhibition zones were measured after incubation at 37 degrees C. B. longum BL03 was used as comparison. The B. longum W11 genome was sequenced on Illumina MiSeq with a 250 PE reads module. After mapping the reads with the reference bacterial genome, the alignment data were processed using FreeBayes software.Results:B. longum BL03 was inhibited by all antibiotics even at the lowest concentration. In contrast, the W11 strain was inhibited by rifampicin, rifabutin, and rifaximin only at the highest concentration (512 g/mL). The genomic analysis showed a mutation into the chromosomal DNA. No transposable elements were found, and the genetic locus was not flanked by close mobile genetic elements.Conclusions:B. longum W11 could be used in combined therapy with rifaximin, thus opening new focused frontiers in the probiotic era while preserving the necessary safety of use for consumers.
机译:目的:研究的目的是明确证明介导长双歧杆菌W11(LMG P-21586)菌株对利福昔明抗性的基因的不可传播性。 ,这在很大程度上归因于肠道菌群的破坏。平行摄入益生菌可能会减少这些事件,即使结果通常很差。在这方面,使用具有抗生素抗性的有益细菌可能是一个值得采取的策略。研究:利福昔明与利福平,利福喷丁和利福布汀并行测试,所有利福霉素均衍生自5种不同浓度。通过Kirby-Bauer的圆盘扩散法进行药敏试验,并且在37℃下孵育后测量抑制区。将长双歧杆菌BL03用作比较。使用250 PE阅读模块在Illumina MiSeq上测序长双歧杆菌W11基因组。在将读数与参考细菌基因组作图后,使用FreeBayes软件处理比对数据。即使在最低浓度下,longum BL03也被所有抗生素抑制。相反,仅在最高浓度(512 g / mL)下,利福平,利福布汀和利福昔明抑制W11菌株。基因组分析显示染色体DNA发生突变。没有发现转座因子,并且遗传位点的侧面没有紧密的移动遗传元件。 Longum W11可与利福昔明联合用于联合治疗,从而在益生菌时代开启了新的关注领域,同时保留了消费者使用所必需的安全性。

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