Four Weeks of Treatment With Rifaximin Fails to Significantly Alter Microbial Diversity in Rectal Samples of HIV-Infected Immune Non-Responders (ACTG A5286) Which May be Attributed to Rectal Swab Use

Brett B. Williams; Stefan J. Green; Ronald J. Bosch; Ellen S. Chan; Jeffrey M. Jacobson; David M. Margolis; Phillip Engen; Alan L. Landay; Cara C. Wilson

doi:10.20411/pai.v4i2.290

Pathogens and Immunity (Sep 2019)

Four Weeks of Treatment With Rifaximin Fails to Significantly Alter Microbial Diversity in Rectal Samples of HIV-Infected Immune Non-Responders (ACTG A5286) Which May be Attributed to Rectal Swab Use

Brett B. Williams,
Stefan J. Green,
Ronald J. Bosch,
Ellen S. Chan,
Jeffrey M. Jacobson,
David M. Margolis,
Phillip Engen,
Alan L. Landay,
Cara C. Wilson

Affiliations

Brett B. Williams: Division of Infectious Disease; Rush University Medical Center; Chicago, Illinois
Stefan J. Green: Sequencing Core; University of Illinois at Chicago; Chicago, Illinois
Ronald J. Bosch: Center for Biostatistics in AIDS Research; Harvard School of Public Health; Boston, Massachusetts
Ellen S. Chan: Center for Biostatistics in AIDS Research; Harvard School of Public Health; Boston, Massachusetts
Jeffrey M. Jacobson: Division of Infectious Diseases and HIV; Drexel University; Philadelphia, Pennsylvania
David M. Margolis: Department of Medicine; University of North Carolina; Chapel Hill, North Carolina
Phillip Engen: Division of Gastroenterology, Hepatology and Nutrition; Department of Medicine; Rush University Medical Center; Chicago, Illinois
Alan L. Landay: Department of Immunology and Microbiology; Rush University Medical Center; Chicago, Illinois
Cara C. Wilson: Department of Medicine; University of Colorado at Denver; Aurora, Colorado

DOI: https://doi.org/10.20411/pai.v4i2.290
Journal volume & issue: Vol. 4, no. 2
pp. 235 – 250

Abstract

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Introduction: HIV-infected individuals have evidence of intestinal microbial translocation which is associated with immune activation and unfavorable clinical outcomes. Rifaximin, a non-absorbable antibiotic which reduces microbial translocation in other disease states, was shown to have a marginal beneficial effect on microbial translocation, T-cell activation, and inflammation in a multisite randomized trial (ACTG A5286; NCT01466595) of HIV-infected persons with poor immunologic recovery receiving ART. Here, we report analysis of the rectal microbiome changes associated with that trial. Methods: HIV-1-infected individuals receiving ART with CD4-T cell count <350cells/mm3 and viral suppression were randomized 2:1 to rifaximin or no therapy for 4 weeks. Rectal swabs were collected at baseline (pre-treatment) and at week 4 of rifaximin therapy. Genomic DNA extracted from rectal swab samples was analyzed using high throughput sequencing and quantitative PCR of bacterial 16S ribosomal RNA (rRNA) genes. Results: Forty-eight HIV-infected participants (31 received rifaximin, 17 no treatment) were included. There was broad variability in the recovery of bacterial rRNA from the specimens at baseline. No major significant (FDR P<0.05) effects of rifaximin treatment on alpha- or beta- diversity or individual taxa were observed between or within the treatment arms, with analyses conducted at taxonomic levels from phylum to genus. Conclusions: Rifaximin did not meaningfully alter the diversity or composition of the rectal microbiome of HIV-infected individuals after 4 weeks of therapy, although rectal swab specimens varied widely in their microbial load.

Published in Pathogens and Immunity

ISSN: 2469-2964 (Online)
Publisher: Case Western Reserve University
Country of publisher: United States
LCC subjects: Medicine: Pathology; Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://www.paijournal.com

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