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656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status

BACKGROUND: Extraintestinal E. coli infections, a perennial source of morbidity and mortality, are increasingly difficult to treat due to emerging antibiotic resistance. Within-HH sharing of E. coli strains may contribute to this problem, but is poorly understood. Accordingly, we assessed E. coli st...

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Autores principales: Boettcher, Jessica, Clabots, Connie, Porter, Stephen B, Johnson, James R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6255421/
http://dx.doi.org/10.1093/ofid/ofy210.663
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author Boettcher, Jessica
Clabots, Connie
Porter, Stephen B
Johnson, James R
author_facet Boettcher, Jessica
Clabots, Connie
Porter, Stephen B
Johnson, James R
author_sort Boettcher, Jessica
collection PubMed
description BACKGROUND: Extraintestinal E. coli infections, a perennial source of morbidity and mortality, are increasingly difficult to treat due to emerging antibiotic resistance. Within-HH sharing of E. coli strains may contribute to this problem, but is poorly understood. Accordingly, we assessed E. coli strain sharing within the HHs of veterans with a clinical E. coli isolate, including in relation to FQ resistance and ST131 status. METHODS: Twenty-two veterans with a clinical E. coli isolate (11 FQ-resistant [FQ-R], 11 FQ-susceptible [FQ-S]) and their HH members underwent serial stool sampling (2–6 occasions each). Stool samples were cultured selectively for FQ-S and FQ-R E. coli. Per sample, 10 E. coli colonies underwent PCR-based profiling; one colony per profile underwent pulsotyping and PCR-based ST131 detection, as did all clinical isolates. Each strain’s extent of within-HH sharing and colonization were calculated. RESULTS: Of the 11 FQ-R clinical isolates, seven were ST131 and four non-ST131; all FQ-S clinical isolates were non-ST131. The 22 HHs included 68 total subjects (49 humans, 19 pets), with a per-HH mean of three subjects, 9.5 total fecal samples, and 6.7 unique strains. The index patient’s stool yielded the corresponding clinical strain in 91% of FQ-R HHs, but only 45% of FQ-S HHs. Sharing of the clinical strain occurred in 45% of FQ-R HHs (43% if ST131, 50% if non-ST131), vs. 27% of FQ-S HHs. For the 22 clinical strains, the extent of within-HH sharing and colonization was greater for FQ-R than FQ-S strains (sharing index, 0.45 vs. 0.15; colonization index, 0.47 vs. 0.14). The FQ-R HHs also yielded 12 additional (non-clinical) FQ-R strains, the FQ-S HHs only 1. Non-clinical FQ-R strains colonized much less extensively than FQ-R clinical strains and were not shared between HH members. CONCLUSION: Compared with FQ-S clinical E. coli, FQ-R clinical E. coli more frequently colonize the index patient, are shared among HH members, and co-occur with other HH FQ-R strains, all of which may drive population-level resistance. Given the potentially important clinical implications of within-HH strain sharing and colonization, better understandings are needed of its mechanisms, including characteristics of the strain, host, and gut microbiota. DISCLOSURES: J. R. Johnson, Crucell/Janssen: Consultant, Consulting fee. Allergan: Grant Investigator, Research support. Merck: Grant Investigator, Research support. Melinta: Grant Investigator, Research support. Tetraphase: Grant Investigator, Research support. Syntiron: Consultant, Consulting fee.
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spelling pubmed-62554212018-11-28 656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status Boettcher, Jessica Clabots, Connie Porter, Stephen B Johnson, James R Open Forum Infect Dis Abstracts BACKGROUND: Extraintestinal E. coli infections, a perennial source of morbidity and mortality, are increasingly difficult to treat due to emerging antibiotic resistance. Within-HH sharing of E. coli strains may contribute to this problem, but is poorly understood. Accordingly, we assessed E. coli strain sharing within the HHs of veterans with a clinical E. coli isolate, including in relation to FQ resistance and ST131 status. METHODS: Twenty-two veterans with a clinical E. coli isolate (11 FQ-resistant [FQ-R], 11 FQ-susceptible [FQ-S]) and their HH members underwent serial stool sampling (2–6 occasions each). Stool samples were cultured selectively for FQ-S and FQ-R E. coli. Per sample, 10 E. coli colonies underwent PCR-based profiling; one colony per profile underwent pulsotyping and PCR-based ST131 detection, as did all clinical isolates. Each strain’s extent of within-HH sharing and colonization were calculated. RESULTS: Of the 11 FQ-R clinical isolates, seven were ST131 and four non-ST131; all FQ-S clinical isolates were non-ST131. The 22 HHs included 68 total subjects (49 humans, 19 pets), with a per-HH mean of three subjects, 9.5 total fecal samples, and 6.7 unique strains. The index patient’s stool yielded the corresponding clinical strain in 91% of FQ-R HHs, but only 45% of FQ-S HHs. Sharing of the clinical strain occurred in 45% of FQ-R HHs (43% if ST131, 50% if non-ST131), vs. 27% of FQ-S HHs. For the 22 clinical strains, the extent of within-HH sharing and colonization was greater for FQ-R than FQ-S strains (sharing index, 0.45 vs. 0.15; colonization index, 0.47 vs. 0.14). The FQ-R HHs also yielded 12 additional (non-clinical) FQ-R strains, the FQ-S HHs only 1. Non-clinical FQ-R strains colonized much less extensively than FQ-R clinical strains and were not shared between HH members. CONCLUSION: Compared with FQ-S clinical E. coli, FQ-R clinical E. coli more frequently colonize the index patient, are shared among HH members, and co-occur with other HH FQ-R strains, all of which may drive population-level resistance. Given the potentially important clinical implications of within-HH strain sharing and colonization, better understandings are needed of its mechanisms, including characteristics of the strain, host, and gut microbiota. DISCLOSURES: J. R. Johnson, Crucell/Janssen: Consultant, Consulting fee. Allergan: Grant Investigator, Research support. Merck: Grant Investigator, Research support. Melinta: Grant Investigator, Research support. Tetraphase: Grant Investigator, Research support. Syntiron: Consultant, Consulting fee. Oxford University Press 2018-11-26 /pmc/articles/PMC6255421/ http://dx.doi.org/10.1093/ofid/ofy210.663 Text en © The Author(s) 2018. Published by Oxford University Press on behalf of Infectious Diseases Society of America. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs licence (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial reproduction and distribution of the work, in any medium, provided the original work is not altered or transformed in any way, and that the work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Abstracts
Boettcher, Jessica
Clabots, Connie
Porter, Stephen B
Johnson, James R
656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status
title 656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status
title_full 656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status
title_fullStr 656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status
title_full_unstemmed 656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status
title_short 656. E. coli Clone Sharing and Persistence Within Households (HHs) in Relation to Fluoroquinolone (FQ) Resistance and ST131 Status
title_sort 656. e. coli clone sharing and persistence within households (hhs) in relation to fluoroquinolone (fq) resistance and st131 status
topic Abstracts
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6255421/
http://dx.doi.org/10.1093/ofid/ofy210.663
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