Gut Microbiota as Well as Metabolomes of Wistar Rats Recover within Two Weeks after Doripenem Antibiotic Treatment

Author:

Murali Aishwarya1ORCID,Zickgraf Franziska Maria1,Ternes Philipp2ORCID,Giri Varun1,Cameron Hunter James3,Sperber Saskia1,Haake Volker2,Driemert Peter2,Kamp Hennicke2ORCID,Weyer Dorothee Funk1,Sturla Shana J.4ORCID,Rietjens Ivonne M. G. M.5,van Ravenzwaay Bennard5ORCID

Affiliation:

1. BASF SE, 67056 Ludwigshafen, Germany

2. BASF Metabolome Solutions GmbH, 10589 Berlin, Germany

3. BASF Plant Science LP, Research Triangle Park, Raleigh, NC 27709, USA

4. ETH Zürich, Department of Health Sciences and Technology, Schmelzbergstrasse 9, 8092 Zurich, Switzerland

5. Department of Toxicology, Wageningen University & Research, 6703 HE Wageningen, The Netherlands

Abstract

An understanding of the changes in gut microbiome composition and its associated metabolic functions is important to assess the potential implications thereof on host health. Thus, to elucidate the connection between the gut microbiome and the fecal and plasma metabolomes, two poorly bioavailable carbapenem antibiotics (doripenem and meropenem), were administered in a 28-day oral study to male and female Wistar rats. Additionally, the recovery of the gut microbiome and metabolomes in doripenem-exposed rats were studied one and two weeks after antibiotic treatment (i.e., doripenem-recovery groups). The 16S bacterial community analysis revealed an altered microbial population in all antibiotic treatments and a recovery of bacterial diversity in the doripenem-recovery groups. A similar pattern was observed in the fecal metabolomes of treated animals. In the recovery group, particularly after one week, an over-compensation was observed in fecal metabolites, as they were significantly changed in the opposite direction compared to previously changed metabolites upon 28 days of antibiotic exposure. Key plasma metabolites known to be diagnostic of antibiotic-induced microbial shifts, including indole derivatives, hippuric acid, and bile acids were also affected by the two carbapenems. Moreover, a unique increase in the levels of indole-3-acetic acid in plasma following meropenem treatment was observed. As was observed for the fecal metabolome, an overcompensation of plasma metabolites was observed in the recovery group. The data from this study provides insights into the connectivity of the microbiome and fecal and plasma metabolomes and demonstrates restoration post-antibiotic treatment not only for the microbiome but also for the metabolomes. The importance of overcompensation reactions for health needs further studies.

Funder

European Chemical Industry Council

Publisher

MDPI AG

Subject

Virology,Microbiology (medical),Microbiology

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