Unknown

Dataset Information

0

Activation of HIF-1? and LL-37 by commensal bacteria inhibits Candida albicans colonization.

ABSTRACT: Candida albicans colonization is required for invasive disease. Unlike humans, adult mice with mature intact gut microbiota are resistant to C. albicans gastrointestinal (GI) colonization, but the factors that promote C. albicans colonization resistance are unknown. Here we demonstrate that commensal anaerobic bacteria-specifically clostridial Firmicutes (clusters IV and XIVa) and Bacteroidetes-are critical for maintaining C. albicans colonization resistance in mice. Using Bacteroides thetaiotamicron as a model organism, we find that hypoxia-inducible factor-1? (HIF-1?), a transcription factor important for activating innate immune effectors, and the antimicrobial peptide LL-37 (CRAMP in mice) are key determinants of C. albicans colonization resistance. Although antibiotic treatment enables C. albicans colonization, pharmacologic activation of colonic Hif1a induces CRAMP expression and results in a significant reduction of C. albicans GI colonization and a 50% decrease in mortality from invasive disease. In the setting of antibiotics, Hif1a and Camp (which encodes CRAMP) are required for B. thetaiotamicron-induced protection against C. albicans colonization of the gut. Thus, modulating C. albicans GI colonization by activation of gut mucosal immune effectors may represent a novel therapeutic approach for preventing invasive fungal disease in humans.

SUBMITTER: Fan D 

PROVIDER: S-EPMC4496259 | biostudies-literature | 2015 Jul

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

Activation of HIF-1α and LL-37 by commensal bacteria inhibits Candida albicans colonization.

Fan Di D   Coughlin Laura A LA   Neubauer Megan M MM   Kim Jiwoong J   Kim Min Soo MS   Zhan Xiaowei X   Simms-Waldrip Tiffany R TR   Xie Yang Y   Hooper Lora V LV   Koh Andrew Y AY  

Nature medicine 20150608 7

Candida albicans colonization is required for invasive disease. Unlike humans, adult mice with mature intact gut microbiota are resistant to C. albicans gastrointestinal (GI) colonization, but the factors that promote C. albicans colonization resistance are unknown. Here we demonstrate that commensal anaerobic bacteria-specifically clostridial Firmicutes (clusters IV and XIVa) and Bacteroidetes-are critical for maintaining C. albicans colonization resistance in mice. Using Bacteroides thetaiotam  ...[more]

Similar Datasets

Unknown Human antimicrobial peptide LL-37 inhibits adhesion of Candida albicans by interacting with yeast cell-wall carbohydrates.
| S-EPMC3056723 | biostudies-literature
Unknown HIF-1 mediated activation of antimicrobial peptide LL-37 in type 2 diabetic patients.
| S-EPMC8724101 | biostudies-literature
Unknown Pre-colonization with the commensal fungus Candida albicans reduces murine susceptibility to Clostridium difficile infection.
| S-EPMC6287688 | biostudies-other
Unknown Commensal enteric bacteria lipopolysaccharide impairs host defense against disseminated Candida albicans fungal infection.
| S-EPMC4465067 | biostudies-literature
Unknown Candida albicans Sfp1 Is Involved in the Cell Wall and Endoplasmic Reticulum Stress Responses Induced by Human Antimicrobial Peptide LL-37.
| S-EPMC8508991 | biostudies-literature
Unknown Colonization with the commensal fungus Candida albicans perturbs the gut-brain axis through dysregulation of endocannabinoid signaling.
| S-EPMC7572798 | biostudies-literature
Unknown Metabolic modeling predicts specific gut bacteria as key determinants for Candida albicans colonization levels.
| S-EPMC8115155 | biostudies-literature
Unknown Entinostat up-regulates the CAMP gene encoding LL-37 via activation of STAT3 and HIF-1? transcription factors.
| S-EPMC5025742 | biostudies-other
Unknown Commensal Candida albicans Positively Calibrates Systemic Th17 Immunological Responses.
| S-EPMC6419754 | biostudies-literature
Unknown LL-37 opsonizes and inhibits biofilm formation of Aggregatibacter actinomycetemcomitans at subbactericidal concentrations.
| S-EPMC3811755 | biostudies-literature