Protection of the Human Gut Microbiome From Antibiotics

نویسندگان

  • Jean de Gunzburg
  • Amine Ghozlane
  • Annie Ducher
  • Emmanuelle Le Chatelier
  • Xavier Duval
  • Etienne Ruppé
  • Laurence Armand-Lefevre
  • Frédérique Sablier-Gallis
  • Charles Burdet
  • Loubna Alavoine
  • Elisabeth Chachaty
  • Violaine Augustin
  • Marina Varastet
  • Florence Levenez
  • Sean Kennedy
  • Nicolas Pons
  • France Mentré
  • Antoine Andremont
چکیده

Background Antibiotics are life-saving drugs but severely affect the gut microbiome with short-term consequences including diarrhea and selection of antibiotic-resistant bacteria. Long-term links to allergy and obesity are also suggested. We devised a product, DAV132, and previously showed its ability to deliver a powerful adsorbent, activated charcoal, in the late ileum of human volunteers. Methods We performed a randomized controlled trial in 28 human volunteers treated with a 5-day clinical regimen of the fluoroquinolone antibiotic moxifloxacin in 2 parallel groups, with or without DAV132 coadministration. Two control goups of 8 volunteers each receiving DAV132 alone, or a nonactive substitute, were added. Results The coadministration of DAV132 decreased free moxifloxacin fecal concentrations by 99%, while plasmatic levels were unaffected. Shotgun quantitative metagenomics showed that the richness and composition of the intestinal microbiota were largely preserved in subjects co-treated with DAV132 in addition to moxifloxacin. No adverse effect was observed. In addition, DAV132 efficiently adsorbed a wide range of clinically relevant antibiotics ex vivo. Conclusions DAV132 was highly effective to protect the gut microbiome of moxifloxacin-treated healthy volunteers and may constitute a clinical breakthrough by preventing adverse health consequences of a wide range of antibiotic treatments. Clinical Trials Registration NCT02176005.

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عنوان ژورنال:

دوره 217  شماره 

صفحات  -

تاریخ انتشار 2018