Nextgeneration probiotics targeting Clostridium difficile through precursor-directed antimicrobial biosynthesis

Jennifer K. Spinler; Jennifer Auchtung; Aaron Brown; Prapaporn Boonma; Numan Oezguen; Caná L. Ross; Ruth Ann Luna; Jessica Runge; James Versalovic; Alex Peniche; Sara M. Dann; Robert A. Britton; Anthony Haag; Tor C. Savidge

doi:10.1128/IAI.00303-17

Nextgeneration probiotics targeting Clostridium difficile through precursor-directed antimicrobial biosynthesis

Jennifer K. Spinler, Jennifer Auchtung, Aaron Brown, Prapaporn Boonma, Numan Oezguen, Caná L. Ross, Ruth Ann Luna, Jessica Runge, James Versalovic, Alex Peniche, Sara M. Dann, Robert A. Britton, Anthony Haag, Tor C. Savidge

Research output: Contribution to journal › Article › peer-review

43 Scopus citations

Abstract

Integration of antibiotic and probiotic therapy has the potential to lessen the public health burden of antimicrobial-associated diseases. Clostridium difficile infection (CDI) represents an important example where the rational design of next-generation probiotics is being actively pursued to prevent disease recurrence. Because intrinsic resistance to clinically relevant antibiotics used to treat CDI (vancomycin, metronidazole, and fidaxomicin) is a desired trait in such probiotic species, we screened several bacteria and identified Lactobacillus reuteri to be a promising candidate for adjunct therapy. Human-derived L. reuteri bacteria convert glycerol to the broad-spectrum antimicrobial compound reuterin. When supplemented with glycerol, strains carrying the pocR gene locus were potent reuterin producers, with L. reuteri 17938 inhibiting C. difficile growth at a level on par with the level of growth inhibition by vancomycin. Targeted pocR mutations and complementation studies identified reuterin to be the precursor-induced antimicrobial agent. Pathophysiological relevance was demonstrated when the codelivery of L. reuteri with glycerol was effective against C. difficile colonization in complex human fecal microbial communities, whereas treatment with either glycerol or L. reuteri alone was ineffective. A global unbiased microbiome and metabolomics analysis independently confirmed that glycerol precursor delivery with L. reuteri elicited changes in the composition and function of the human microbial community that preferentially targets C. difficile outgrowth and toxicity, a finding consistent with glycerol fermentation and reuterin production. Antimicrobial resistance has thus been successfully exploited in the natural design of human microbiome evasion of C. difficile, and this method may provide a prototypic precursor-directed probiotic approach. Antibiotic resistance and substrate bioavailability may therefore represent critical new determinants of probiotic efficacy in clinical trials.

Original language	English (US)
Article number	e00303-17
Journal	Infection and Immunity
Volume	85
Issue number	10
DOIs	https://doi.org/10.1128/IAI.00303-17
State	Published - 2017

Keywords

Antimicrobial resistance
Clostridium difficile
Lactobacillus reuteri
Next-generation probiotics
Reuterin

ASJC Scopus subject areas

Parasitology
Microbiology
Immunology
Infectious Diseases

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Spinler, J. K., Auchtung, J., Brown, A., Boonma, P., Oezguen, N., Ross, C. L., Luna, R. A., Runge, J., Versalovic, J., Peniche, A., Dann, S. M., Britton, R. A., Haag, A., & Savidge, T. C. (2017). Nextgeneration probiotics targeting Clostridium difficile through precursor-directed antimicrobial biosynthesis. Infection and Immunity, 85(10), [e00303-17]. https://doi.org/10.1128/IAI.00303-17

Spinler, JK, Auchtung, J, Brown, A, Boonma, P, Oezguen, N, Ross, CL, Luna, RA, Runge, J, Versalovic, J, Peniche, A, Dann, SM, Britton, RA, Haag, A & Savidge, TC 2017, 'Nextgeneration probiotics targeting Clostridium difficile through precursor-directed antimicrobial biosynthesis', Infection and Immunity, vol. 85, no. 10, e00303-17. https://doi.org/10.1128/IAI.00303-17

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title = "Nextgeneration probiotics targeting Clostridium difficile through precursor-directed antimicrobial biosynthesis",

abstract = "Integration of antibiotic and probiotic therapy has the potential to lessen the public health burden of antimicrobial-associated diseases. Clostridium difficile infection (CDI) represents an important example where the rational design of next-generation probiotics is being actively pursued to prevent disease recurrence. Because intrinsic resistance to clinically relevant antibiotics used to treat CDI (vancomycin, metronidazole, and fidaxomicin) is a desired trait in such probiotic species, we screened several bacteria and identified Lactobacillus reuteri to be a promising candidate for adjunct therapy. Human-derived L. reuteri bacteria convert glycerol to the broad-spectrum antimicrobial compound reuterin. When supplemented with glycerol, strains carrying the pocR gene locus were potent reuterin producers, with L. reuteri 17938 inhibiting C. difficile growth at a level on par with the level of growth inhibition by vancomycin. Targeted pocR mutations and complementation studies identified reuterin to be the precursor-induced antimicrobial agent. Pathophysiological relevance was demonstrated when the codelivery of L. reuteri with glycerol was effective against C. difficile colonization in complex human fecal microbial communities, whereas treatment with either glycerol or L. reuteri alone was ineffective. A global unbiased microbiome and metabolomics analysis independently confirmed that glycerol precursor delivery with L. reuteri elicited changes in the composition and function of the human microbial community that preferentially targets C. difficile outgrowth and toxicity, a finding consistent with glycerol fermentation and reuterin production. Antimicrobial resistance has thus been successfully exploited in the natural design of human microbiome evasion of C. difficile, and this method may provide a prototypic precursor-directed probiotic approach. Antibiotic resistance and substrate bioavailability may therefore represent critical new determinants of probiotic efficacy in clinical trials.",

keywords = "Antimicrobial resistance, Clostridium difficile, Lactobacillus reuteri, Next-generation probiotics, Reuterin",

author = "Spinler, {Jennifer K.} and Jennifer Auchtung and Aaron Brown and Prapaporn Boonma and Numan Oezguen and Ross, {Can{\'a} L.} and Luna, {Ruth Ann} and Jessica Runge and James Versalovic and Alex Peniche and Dann, {Sara M.} and Britton, {Robert A.} and Anthony Haag and Savidge, {Tor C.}",

note = "Funding Information: This work was supported by the National Institutes of Health, including a pilot funding award through the Texas Medical Center Digestive Disease Center (P30 DK56338) (J.K.S.), the National Institute of Allergy and Infectious Diseases (NIAID) R01 AI10094001 (T.C.S.), U01 AI124290-01 (T.C.S.), and 5U19AI090872-02 (R.A.B.), and the Institute for Translational Sciences at the University of Texas Medical Branch through Clinical and Translational Science Award UL1TR000071 (S.M.D.). Publisher Copyright: {\textcopyright} 2017 American Society for Microbiology.",

year = "2017",

doi = "10.1128/IAI.00303-17",

language = "English (US)",

volume = "85",

journal = "Infection and Immunity",

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AU - Spinler, Jennifer K.

AU - Auchtung, Jennifer

AU - Brown, Aaron

AU - Boonma, Prapaporn

AU - Oezguen, Numan

AU - Ross, Caná L.

AU - Luna, Ruth Ann

AU - Runge, Jessica

AU - Versalovic, James

AU - Peniche, Alex

AU - Dann, Sara M.

AU - Britton, Robert A.

AU - Haag, Anthony

AU - Savidge, Tor C.

N1 - Funding Information: This work was supported by the National Institutes of Health, including a pilot funding award through the Texas Medical Center Digestive Disease Center (P30 DK56338) (J.K.S.), the National Institute of Allergy and Infectious Diseases (NIAID) R01 AI10094001 (T.C.S.), U01 AI124290-01 (T.C.S.), and 5U19AI090872-02 (R.A.B.), and the Institute for Translational Sciences at the University of Texas Medical Branch through Clinical and Translational Science Award UL1TR000071 (S.M.D.). Publisher Copyright: © 2017 American Society for Microbiology.

PY - 2017

Y1 - 2017

N2 - Integration of antibiotic and probiotic therapy has the potential to lessen the public health burden of antimicrobial-associated diseases. Clostridium difficile infection (CDI) represents an important example where the rational design of next-generation probiotics is being actively pursued to prevent disease recurrence. Because intrinsic resistance to clinically relevant antibiotics used to treat CDI (vancomycin, metronidazole, and fidaxomicin) is a desired trait in such probiotic species, we screened several bacteria and identified Lactobacillus reuteri to be a promising candidate for adjunct therapy. Human-derived L. reuteri bacteria convert glycerol to the broad-spectrum antimicrobial compound reuterin. When supplemented with glycerol, strains carrying the pocR gene locus were potent reuterin producers, with L. reuteri 17938 inhibiting C. difficile growth at a level on par with the level of growth inhibition by vancomycin. Targeted pocR mutations and complementation studies identified reuterin to be the precursor-induced antimicrobial agent. Pathophysiological relevance was demonstrated when the codelivery of L. reuteri with glycerol was effective against C. difficile colonization in complex human fecal microbial communities, whereas treatment with either glycerol or L. reuteri alone was ineffective. A global unbiased microbiome and metabolomics analysis independently confirmed that glycerol precursor delivery with L. reuteri elicited changes in the composition and function of the human microbial community that preferentially targets C. difficile outgrowth and toxicity, a finding consistent with glycerol fermentation and reuterin production. Antimicrobial resistance has thus been successfully exploited in the natural design of human microbiome evasion of C. difficile, and this method may provide a prototypic precursor-directed probiotic approach. Antibiotic resistance and substrate bioavailability may therefore represent critical new determinants of probiotic efficacy in clinical trials.

AB - Integration of antibiotic and probiotic therapy has the potential to lessen the public health burden of antimicrobial-associated diseases. Clostridium difficile infection (CDI) represents an important example where the rational design of next-generation probiotics is being actively pursued to prevent disease recurrence. Because intrinsic resistance to clinically relevant antibiotics used to treat CDI (vancomycin, metronidazole, and fidaxomicin) is a desired trait in such probiotic species, we screened several bacteria and identified Lactobacillus reuteri to be a promising candidate for adjunct therapy. Human-derived L. reuteri bacteria convert glycerol to the broad-spectrum antimicrobial compound reuterin. When supplemented with glycerol, strains carrying the pocR gene locus were potent reuterin producers, with L. reuteri 17938 inhibiting C. difficile growth at a level on par with the level of growth inhibition by vancomycin. Targeted pocR mutations and complementation studies identified reuterin to be the precursor-induced antimicrobial agent. Pathophysiological relevance was demonstrated when the codelivery of L. reuteri with glycerol was effective against C. difficile colonization in complex human fecal microbial communities, whereas treatment with either glycerol or L. reuteri alone was ineffective. A global unbiased microbiome and metabolomics analysis independently confirmed that glycerol precursor delivery with L. reuteri elicited changes in the composition and function of the human microbial community that preferentially targets C. difficile outgrowth and toxicity, a finding consistent with glycerol fermentation and reuterin production. Antimicrobial resistance has thus been successfully exploited in the natural design of human microbiome evasion of C. difficile, and this method may provide a prototypic precursor-directed probiotic approach. Antibiotic resistance and substrate bioavailability may therefore represent critical new determinants of probiotic efficacy in clinical trials.

KW - Antimicrobial resistance

KW - Clostridium difficile

KW - Lactobacillus reuteri

KW - Next-generation probiotics

KW - Reuterin

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ER -

Nextgeneration probiotics targeting Clostridium difficile through precursor-directed antimicrobial biosynthesis

Abstract

Keywords

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