Mechanism underlying prolongevity induced by bifidobacteria in Caenorhabditis elegans

Komura, Tomomi; Ikeda, Takanori; Yasui, Chikako; Saeki, Shigeru; Nishikawa, Yoshikazu

doi:10.1007/s10522-012-9411-6

Cited by 86 publications

(92 citation statements)

References 58 publications

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“…These pathways include: 1) P38-MAPK pathway, 2) TGF-β pathway, and 3) Insulin/IGF-like pathway. Lactobacillus can also induce C. elegans ’s host response [43], [44]. In the present study, L. zeae LB1 was able to effectively prevent C. elegans from death caused by ETEC JG280 or individual enterotoxin clones (Table 1, Fig.…”

Section: Discussionsupporting

confidence: 51%

Lactobacillus zeae Protects Caenorhabditis elegans from Enterotoxigenic Escherichia coli-Caused Death by Inhibiting Enterotoxin Gene Expression of the Pathogen

Zhou

et al. 2014

PLoS ONE

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BackgroundThe nematode Caenorhabditis elegans has become increasingly used for screening antimicrobials and probiotics for pathogen control. It also provides a useful tool for studying microbe-host interactions. This study has established a C. elegans life-span assay to preselect probiotic bacteria for controlling K88+ enterotoxigenic Escherichia coli (ETEC), a pathogen causing pig diarrhea, and has determined a potential mechanism underlying the protection provided by Lactobacillus.Methodology/Principal FindingsLife-span of C. elegans was used to measure the response of worms to ETEC infection and protection provided by lactic acid-producing bacteria (LAB). Among 13 LAB isolates that varied in their ability to protect C. elegans from death induced by ETEC strain JG280, Lactobacillus zeae LB1 offered the highest level of protection (86%). The treatment with Lactobacillus did not reduce ETEC JG280 colonization in the nematode intestine. Feeding E. coli strain JFF4 (K88+ but lacking enterotoxin genes of estA, estB, and elt) did not cause death of worms. There was a significant increase in gene expression of estA, estB, and elt during ETEC JG280 infection, which was remarkably inhibited by isolate LB1. The clone with either estA or estB expressed in E. coli DH5α was as effective as ETEC JG280 in killing the nematode. However, the elt clone killed only approximately 40% of worms. The killing by the clones could also be prevented by isolate LB1. The same isolate only partially inhibited the gene expression of enterotoxins in both ETEC JG280 and E. coli DH5α in-vitro.Conclusions/SignificanceThe established life-span assay can be used for studies of probiotics to control ETEC (for effective selection and mechanistic studies). Heat-stable enterotoxins appeared to be the main factors responsible for the death of C. elegans. Inhibition of ETEC enterotoxin production, rather than interference of its intestinal colonization, appears to be the mechanism of protection offered by Lactobacillus.

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Section: Discussionsupporting

confidence: 51%

Lactobacillus zeae Protects Caenorhabditis elegans from Enterotoxigenic Escherichia coli-Caused Death by Inhibiting Enterotoxin Gene Expression of the Pathogen

Zhou

et al. 2014

PLoS ONE

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“…According to these authors and in agreement with our own results, TOL-1 has a direct role in the immune response to certain gram negative bacteria. It was reported that worms fed the gram positive Bifidobacterium infantis lived longer than E. coli fed worms, and that tol-1 mutant worms lived longer on B. infantis than WT worms [57]. We speculate that TOL-1 functions to protect C. elegans against gram negative specific factors, but that the activity of this protection system might be detrimental as when TOL-1 is not functional and the gram negative threat is not present (worms are fed gram positive bacteria), worms live longer than WT worms.…”

Section: Discussionmentioning

confidence: 99%

Dietary and microbiome factors determine longevity in Caenorhabditis elegans

Sánchez-Blanco

Rodríguez-Matellán

Gonzaléz-Paramás

et al. 2016

Aging

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Diet composition affects organismal health. Nutrient uptake depends on the microbiome. Caenorhabditis elegans fed a Bacillus subtilis diet live longer than those fed the standard Escherichia coli diet. Here we report that this longevity difference is primarily caused by dietary coQ, an antioxidant synthesized by E. coli but not by B. subtilis. CoQ-supplemented E. coli fed worms have a lower oxidation state yet live shorter than coQ-less B. subtilis fed worms. We showed that mutations affecting longevity for E. coli fed worms do not always lead to similar effects when worms are fed B. subtilis. We propose that coQ supplementation by the E. coli diet alters the worm cellular REDOX homeostasis, thus decreasing longevity. Our results highlight the importance of microbiome factors in longevity, argue that antioxidant supplementation can be detrimental, and suggest that the C. elegans standard E. coli diet can alter the effect of signaling pathways on longevity.

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“…A study examining the effect of Bifidobacterium infantis on C. elegans lifespan found a modest dose‐dependent lifespan extension when B. infantis was added to OP50 (Komura et al ., ). The authors also report an extension in healthspan of worms fed B. infantis , defined by locomotion and co‐ordination.…”

Section: Probiotic Effects On Lifespanmentioning

confidence: 97%

“…2A). Several studies Fasseas et al, 2013;Komura et al, 2013;MacNeil et al, 2013) have ruled out the involvement of DAF-16 in probiotic-mediated lifespan extension, indicating that there are multiple independent pathways affecting C. elegans longevity.…”

Section: Pathogen Protective Effectsmentioning

confidence: 99%

Commensals, probiotics and pathogens in theCaenorhabditis elegansmodel

Clark

Hodgkin

2013

Cell Microbiol

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SummaryCaenorhabditis elegans is a useful model host for a wide variety of microorganisms that have implications for human health. Recent surveys of mammalian and metazoan microbiota demonstrate the often profound effects of gut commensal bacteria on host lifespan, health and development. Work using C. elegans has revealed the surprising extent to which bacterial metabolism can interact with host pathways with examples from Escherichia coli folate metabolism and Bacillus subtilis nitric oxide synthesis. The C. elegans model has also shed light on the mechanisms by which probiotic bacteria influence lifespan.

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Mechanism underlying prolongevity induced by bifidobacteria in Caenorhabditis elegans

Cited by 86 publications

References 58 publications

Lactobacillus zeae Protects Caenorhabditis elegans from Enterotoxigenic Escherichia coli-Caused Death by Inhibiting Enterotoxin Gene Expression of the Pathogen

Lactobacillus zeae Protects Caenorhabditis elegans from Enterotoxigenic Escherichia coli-Caused Death by Inhibiting Enterotoxin Gene Expression of the Pathogen

Dietary and microbiome factors determine longevity in Caenorhabditis elegans

Commensals, probiotics and pathogens in theCaenorhabditis elegansmodel

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