Gut microbiota disturbance during antibiotic therapy: a multi-omic approach

Ana Elena Pérez-Cobas; María José Gosalbes; Anette Friedrichs; Henrik Knecht; Alejandro Artacho; Kathleen Eismann; Wolfgang Otto; David Rojo; Rafael Bargiela; Martin von Bergen; Sven C Neulinger; Carolin Däumer; Femke-Anouska Heinsen; Amparo Latorre; Coral Barbas; Jana Seifert; Vitor Martins Dos Santos; Stephan J Ott; Manuel Ferrer; Andrés Moya

doi:10.1136/gutjnl-2012-303184

Gut microbiota disturbance during antibiotic therapy: a multi-omic approach

Ana Elena Pérez-Cobas, María José Gosalbes, Anette Friedrichs, Henrik Knecht, Alejandro Artacho, Kathleen Eismann, Wolfgang Otto, David Rojo, Rafael Bargiela, Martin von Bergen, Sven C Neulinger, Carolin Däumer, Femke-Anouska Heinsen, Amparo Latorre, Coral Barbas, Jana Seifert, Vitor Martins Dos Santos, Stephan J Ott, Manuel Ferrer, Andrés Moya

Department of Chemistry and Bioscience

Research output: Contribution to journal › Journal article › Research › peer-review

409 Citations (Scopus)

Abstract

OBJECTIVE: Antibiotic (AB) usage strongly affects microbial intestinal metabolism and thereby impacts human health. Understanding this process and the underlying mechanisms remains a major research goal. Accordingly, we conducted the first comparative omic investigation of gut microbial communities in faecal samples taken at multiple time points from an individual subjected to β-lactam therapy. METHODS: The total (16S rDNA) and active (16S rRNA) microbiota, metagenome, metatranscriptome (mRNAs), metametabolome (high-performance liquid chromatography coupled to electrospray ionisation and quadrupole time-of-flight mass spectrometry) and metaproteome (ultra high performing liquid chromatography coupled to an Orbitrap MS(2) instrument [UPLC-LTQ Orbitrap-MS/MS]) of a patient undergoing AB therapy for 14 days were evaluated. RESULTS: Apparently oscillatory population dynamics were observed, with an early reduction in Gram-negative organisms (day 6) and an overall collapse in diversity and possible further colonisation by 'presumptive' naturally resistant bacteria (day 11), followed by the re-growth of Gram-positive species (day 14). During this process, the maximum imbalance in the active microbial fraction occurred later (day 14) than the greatest change in the total microbial fraction, which reached a minimum biodiversity and richness on day 11; additionally, major metabolic changes occurred at day 6. Gut bacteria respond to ABs early by activating systems to avoid the antimicrobial effects of the drugs, while 'presumptively' attenuating their overall energetic metabolic status and the capacity to transport and metabolise bile acid, cholesterol, hormones and vitamins; host-microbial interactions significantly improved after treatment cessation. CONCLUSIONS: This proof-of-concept study provides an extensive description of gut microbiota responses to follow-up β-lactam therapy. The results demonstrate that ABs targeting specific pathogenic infections and diseases may alter gut microbial ecology and interactions with host metabolism at a much higher level than previously assumed.

Original language	English
Journal	Gut
Volume	62
Pages (from-to)	1591-1601
Number of pages	11
ISSN	0017-5749
DOIs	https://doi.org/10.1136/gutjnl-2012-303184
Publication status	Published - 2013

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Pérez-Cobas, A. E., Gosalbes, M. J., Friedrichs, A., Knecht, H., Artacho, A., Eismann, K., Otto, W., Rojo, D., Bargiela, R., von Bergen, M., Neulinger, S. C., Däumer, C., Heinsen, F-A., Latorre, A., Barbas, C., Seifert, J., Dos Santos, V. M., Ott, S. J., Ferrer, M., & Moya, A. (2013). Gut microbiota disturbance during antibiotic therapy: a multi-omic approach. Gut, 62, 1591-1601. https://doi.org/10.1136/gutjnl-2012-303184

@article{4c7162d59e4a42bb92abd71afe4e749f,

title = "Gut microbiota disturbance during antibiotic therapy: a multi-omic approach",

abstract = "OBJECTIVE: Antibiotic (AB) usage strongly affects microbial intestinal metabolism and thereby impacts human health. Understanding this process and the underlying mechanisms remains a major research goal. Accordingly, we conducted the first comparative omic investigation of gut microbial communities in faecal samples taken at multiple time points from an individual subjected to β-lactam therapy. METHODS: The total (16S rDNA) and active (16S rRNA) microbiota, metagenome, metatranscriptome (mRNAs), metametabolome (high-performance liquid chromatography coupled to electrospray ionisation and quadrupole time-of-flight mass spectrometry) and metaproteome (ultra high performing liquid chromatography coupled to an Orbitrap MS(2) instrument [UPLC-LTQ Orbitrap-MS/MS]) of a patient undergoing AB therapy for 14 days were evaluated. RESULTS: Apparently oscillatory population dynamics were observed, with an early reduction in Gram-negative organisms (day 6) and an overall collapse in diversity and possible further colonisation by 'presumptive' naturally resistant bacteria (day 11), followed by the re-growth of Gram-positive species (day 14). During this process, the maximum imbalance in the active microbial fraction occurred later (day 14) than the greatest change in the total microbial fraction, which reached a minimum biodiversity and richness on day 11; additionally, major metabolic changes occurred at day 6. Gut bacteria respond to ABs early by activating systems to avoid the antimicrobial effects of the drugs, while 'presumptively' attenuating their overall energetic metabolic status and the capacity to transport and metabolise bile acid, cholesterol, hormones and vitamins; host-microbial interactions significantly improved after treatment cessation. CONCLUSIONS: This proof-of-concept study provides an extensive description of gut microbiota responses to follow-up β-lactam therapy. The results demonstrate that ABs targeting specific pathogenic infections and diseases may alter gut microbial ecology and interactions with host metabolism at a much higher level than previously assumed.",

author = "P{\'e}rez-Cobas, {Ana Elena} and Gosalbes, {Mar{\'i}a Jos{\'e}} and Anette Friedrichs and Henrik Knecht and Alejandro Artacho and Kathleen Eismann and Wolfgang Otto and David Rojo and Rafael Bargiela and {von Bergen}, Martin and Neulinger, {Sven C} and Carolin D{\"a}umer and Femke-Anouska Heinsen and Amparo Latorre and Coral Barbas and Jana Seifert and {Dos Santos}, {Vitor Martins} and Ott, {Stephan J} and Manuel Ferrer and Andr{\'e}s Moya",

year = "2013",

doi = "10.1136/gutjnl-2012-303184",

language = "English",

volume = "62",

pages = "1591--1601",

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Pérez-Cobas, AE, Gosalbes, MJ, Friedrichs, A, Knecht, H, Artacho, A, Eismann, K, Otto, W, Rojo, D, Bargiela, R, von Bergen, M, Neulinger, SC, Däumer, C, Heinsen, F-A, Latorre, A, Barbas, C, Seifert, J, Dos Santos, VM, Ott, SJ, Ferrer, M & Moya, A 2013, 'Gut microbiota disturbance during antibiotic therapy: a multi-omic approach', Gut, vol. 62, pp. 1591-1601. https://doi.org/10.1136/gutjnl-2012-303184

TY - JOUR

T1 - Gut microbiota disturbance during antibiotic therapy

T2 - a multi-omic approach

AU - Pérez-Cobas, Ana Elena

AU - Gosalbes, María José

AU - Friedrichs, Anette

AU - Knecht, Henrik

AU - Artacho, Alejandro

AU - Eismann, Kathleen

AU - Otto, Wolfgang

AU - Rojo, David

AU - Bargiela, Rafael

AU - von Bergen, Martin

AU - Neulinger, Sven C

AU - Däumer, Carolin

AU - Heinsen, Femke-Anouska

AU - Latorre, Amparo

AU - Barbas, Coral

AU - Seifert, Jana

AU - Dos Santos, Vitor Martins

AU - Ott, Stephan J

AU - Ferrer, Manuel

AU - Moya, Andrés

PY - 2013

Y1 - 2013

N2 - OBJECTIVE: Antibiotic (AB) usage strongly affects microbial intestinal metabolism and thereby impacts human health. Understanding this process and the underlying mechanisms remains a major research goal. Accordingly, we conducted the first comparative omic investigation of gut microbial communities in faecal samples taken at multiple time points from an individual subjected to β-lactam therapy. METHODS: The total (16S rDNA) and active (16S rRNA) microbiota, metagenome, metatranscriptome (mRNAs), metametabolome (high-performance liquid chromatography coupled to electrospray ionisation and quadrupole time-of-flight mass spectrometry) and metaproteome (ultra high performing liquid chromatography coupled to an Orbitrap MS(2) instrument [UPLC-LTQ Orbitrap-MS/MS]) of a patient undergoing AB therapy for 14 days were evaluated. RESULTS: Apparently oscillatory population dynamics were observed, with an early reduction in Gram-negative organisms (day 6) and an overall collapse in diversity and possible further colonisation by 'presumptive' naturally resistant bacteria (day 11), followed by the re-growth of Gram-positive species (day 14). During this process, the maximum imbalance in the active microbial fraction occurred later (day 14) than the greatest change in the total microbial fraction, which reached a minimum biodiversity and richness on day 11; additionally, major metabolic changes occurred at day 6. Gut bacteria respond to ABs early by activating systems to avoid the antimicrobial effects of the drugs, while 'presumptively' attenuating their overall energetic metabolic status and the capacity to transport and metabolise bile acid, cholesterol, hormones and vitamins; host-microbial interactions significantly improved after treatment cessation. CONCLUSIONS: This proof-of-concept study provides an extensive description of gut microbiota responses to follow-up β-lactam therapy. The results demonstrate that ABs targeting specific pathogenic infections and diseases may alter gut microbial ecology and interactions with host metabolism at a much higher level than previously assumed.

AB - OBJECTIVE: Antibiotic (AB) usage strongly affects microbial intestinal metabolism and thereby impacts human health. Understanding this process and the underlying mechanisms remains a major research goal. Accordingly, we conducted the first comparative omic investigation of gut microbial communities in faecal samples taken at multiple time points from an individual subjected to β-lactam therapy. METHODS: The total (16S rDNA) and active (16S rRNA) microbiota, metagenome, metatranscriptome (mRNAs), metametabolome (high-performance liquid chromatography coupled to electrospray ionisation and quadrupole time-of-flight mass spectrometry) and metaproteome (ultra high performing liquid chromatography coupled to an Orbitrap MS(2) instrument [UPLC-LTQ Orbitrap-MS/MS]) of a patient undergoing AB therapy for 14 days were evaluated. RESULTS: Apparently oscillatory population dynamics were observed, with an early reduction in Gram-negative organisms (day 6) and an overall collapse in diversity and possible further colonisation by 'presumptive' naturally resistant bacteria (day 11), followed by the re-growth of Gram-positive species (day 14). During this process, the maximum imbalance in the active microbial fraction occurred later (day 14) than the greatest change in the total microbial fraction, which reached a minimum biodiversity and richness on day 11; additionally, major metabolic changes occurred at day 6. Gut bacteria respond to ABs early by activating systems to avoid the antimicrobial effects of the drugs, while 'presumptively' attenuating their overall energetic metabolic status and the capacity to transport and metabolise bile acid, cholesterol, hormones and vitamins; host-microbial interactions significantly improved after treatment cessation. CONCLUSIONS: This proof-of-concept study provides an extensive description of gut microbiota responses to follow-up β-lactam therapy. The results demonstrate that ABs targeting specific pathogenic infections and diseases may alter gut microbial ecology and interactions with host metabolism at a much higher level than previously assumed.

U2 - 10.1136/gutjnl-2012-303184

DO - 10.1136/gutjnl-2012-303184

M3 - Journal article

C2 - 23236009

SN - 0017-5749

VL - 62

SP - 1591

EP - 1601

JO - Gut

JF - Gut

ER -

Gut microbiota disturbance during antibiotic therapy: a multi-omic approach

Abstract

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