Metagenomic Analysis of the Stool Microbiome in Patients Receiving Allogeneic Stem Cell Transplantation: Loss of Diversity Is Associated with Use of Systemic Antibiotics and More Pronounced in Gastrointestinal Graft-versus-Host Disease

Ernst Holler; Peter Butzhammer; Karin Schmid‐Zalaudek; Christian Hundsrucker; Josef Koestler; Katrin Peter; Wentao Zhu; Daniela Sporrer; Thomas Hehlgans; Marina Kreutz; Barbara Holler; Daniel Wolff; Matthias Edinger; Reinhard Andreesen; John E. Levine; James L.M. Ferrara; André Gessner; Rainer Spang; Peter J. Oefner

doi:10.1016/j.bbmt.2014.01.030

Metagenomic Analysis of the Stool Microbiome in Patients Receiving Allogeneic Stem Cell Transplantation: Loss of Diversity Is Associated with Use of Systemic Antibiotics and More Pronounced in Gastrointestinal Graft-versus-Host Disease

Ernst Holler(University Hospital Regensburg), Peter Butzhammer(University of Regensburg), Karin Schmid‐Zalaudek(University Hospital Regensburg), Christian Hundsrucker(University of Regensburg), Josef Koestler, Katrin Peter(University Hospital Regensburg), Wentao Zhu(University of Regensburg), Daniela Sporrer(University Hospital Regensburg), Thomas Hehlgans(University of Regensburg), Marina Kreutz(University Hospital Regensburg), Barbara Holler(University Hospital Regensburg), Daniel Wolff(University Hospital Regensburg), Matthias Edinger(University Hospital Regensburg), Reinhard Andreesen(University Hospital Regensburg), John E. Levine(University of Michigan–Ann Arbor), James L.M. Ferrara(University of Michigan–Ann Arbor), André Gessner, Rainer Spang(University of Regensburg), Peter J. Oefner(University of Regensburg)

Biology of Blood and Marrow Transplantation

February 2, 2014

10.1016/j.bbmt.2014.01.030

Cited by 542Open Access

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Abstract

Next-generation sequencing of the hypervariable V3 region of the 16s rRNA gene isolated from serial stool specimens collected from 31 patients receiving allogeneic stem cell transplantation (SCT) was performed to elucidate variations in the composition of the intestinal microbiome in the course of allogeneic SCT. Metagenomic analysis was complemented by strain-specific enterococcal PCR and indirect assessment of bacterial load by liquid chromatography-tandem mass spectrometry of urinary indoxyl sulfate. At the time of admission, patients showed a predominance of commensal bacteria. After transplantation, a relative shift toward enterococci was observed, which was more pronounced under antibiotic prophylaxis and treatment of neutropenic infections. The shift was particularly prominent in patients that developed subsequently or suffered from active gastrointestinal (GI) graft-versus-host disease (GVHD). The mean proportion of enterococci in post-transplant stool specimens was 21% in patients who did not develop GI GVHD as compared with 46% in those that subsequently developed GI GVHD and 74% at the time of active GVHD. Enterococcal PCR confirmed predominance of Enterococcus faecium or both E. faecium and Enterococcus faecalis in these specimens. As a consequence of the loss of bacterial diversity, mean urinary indoxyl sulfate levels dropped from 42.5 ± 11 μmol/L to 11.8 ± 2.8 μmol/L in all post-transplant samples and to 3.5 ± 3 μmol/L in samples from patients with active GVHD. Our study reveals major microbiome shifts in the course of allogeneic SCT that occur in the period of antibiotic treatment but are more prominent in association with GI GVHD. Our data indicate early microbiome shifts and a loss of diversity of the intestinal microbiome that may affect intestinal inflammation in the setting of allogeneic SCT.

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