Secretion of microbicidal α-defensins by intestinal Paneth cells in response to bacteria

Ayabe, Tokiyoshi; Satchell, Donald P.; Wilson, Carole L.; Parks, William C.; Selsted, Michael E.; Ouellette, André J.

doi:10.1038/77783

Cited by 960 publications

(861 citation statements)

References 46 publications

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“…TLR ligation is at least partly responsible for the NF-kB-dependent expression of defensinscationic peptides that exert direct bactericidal activity by inducing membrane permeabilization. Small intestinal Paneth cells, for example, release large amounts of a-defensins into the intestinal lumen following exposure to a variety of bacteria/bacterial products (Ayabe et al, 2000). The production of antimicrobial nitrogen and oxygen species, which are acutely toxic to a variety of microbes, augments the activity of antimicrobial peptides.…”

Section: Immediate Antimicrobial Responsesmentioning

confidence: 99%

NF-κB and the immune response

2006

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Section: Immediate Antimicrobial Responsesmentioning

confidence: 99%

NF-κB and the immune response

2006

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“…Among naturally occurring AMPs, defensins form a unique and principle family of cysteine rich cationic polypeptides with 3 or 4 disulfide bridges [6]. Mouse enteric alpha-defensins called cryptdins are expressed in the granules of Paneth cells and are secreted into the lumen of intestinal crypts in response to bacterial stimuli [7]. Cryptdins are broad-spectrum AMPs due to their ability to kill various bacteria [8][9][10], parasites [11] and enveloped viruses [12] in vitro.…”

Section: Introductionmentioning

confidence: 99%

Efficacy of Cryptdin-2 as an Adjunct to Antibiotics from Various Generations Against Salmonella

2014

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Emerging drug resistance in Salmonella coupled with the recent poor success rate of antibiotic discovery programs of the pharmaceutical industry is a cause for significant concern. It has forced the scientific community to look for alternative new classes of antimicrobial compounds. In this context, combinations of antimicrobial peptides (AMPs) and conventional antibiotics have gained interest owing to their versatile applications. The present study was therefore planned to evaluate the synergistic effects, if any, of cryptdin-2, a mouse Paneth cell alphadefensin, in combination with four different antibiotics i.e. ciprofloxacin, ceftriaxone, cefotaxime and chloramphenicol, which are conventionally used against Salmonella. Minimum bactericidal concentrations of the selected antimicrobial agents were determined by micro and macro broth dilution assays. In-vitro synergy between the agents was evaluated by fractional bactericidal concentration index (checkerboard test) and time-kill assay. Cryptdin-2-ciprofloxacin, cryptdin-2-ceftriaxone and cryptdin-2-cefotaxime combinations were found synergistic as evident by in vitro assays. This synergism provides an additional therapeutic choice by allowing the use of conventional antibiotics in conjunction with AMPs against MDR Salmonella.

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“…1 These cells sense bacterial presence and secrete granules containing antimicrobial peptides, including lysozyme, RegIII␥, and cryptdins (the murine counterparts of human ␣-defensins) both constitutively and in response to activation by bacteria or their products. 2 Using a murine cell ablation model, Paneth cells were shown to be crucial in host protection against invasion of both commensal and pathogenic microbiota. 3 In addition, our group has recently shown the additive importance of Paneth cells in preventing bacterial translocation in situations of physical intestinal barrier loss.…”

mentioning

confidence: 99%

Starvation Compromises Paneth Cells

Hodin

Lenaerts

Grootjans

et al. 2011

The American Journal of Pathology

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The intestine is challenged with the task of protecting the body's internal milieu against bacterial invasion. To this end, the gut is equipped with an epithelial lining connected by tight junctions, a mucus layer, gut-associated lymphoid tissue, and Paneth cells. Paneth cells are highly specialized epithelial cells located in the crypts of the small intestine, and play an important role in gut innate immunity. 1 These cells sense bacterial presence and secrete granules containing antimicrobial peptides, including lysozyme, RegIII␥, and cryptdins (the murine counterparts of human ␣-defensins) both constitutively and in response to activation by bacteria or their products. 2 Using a murine cell ablation model, Paneth cells were shown to be crucial in host protection against invasion of both commensal and pathogenic microbiota. 3 In addition, our group has recently shown the additive importance of Paneth cells in preventing bacterial translocation in situations of physical intestinal barrier loss. 4 Enteral starvation and total parenteral nutrition, as applied to critically ill patients, are reported to result in increased gut wall permeability, a compromised immune system, and bacterial translocation. 5-10 Because autophagy, a process induced on starvation, 11-13 influences the generation of Paneth cell granules, 14 we hypothesize that enteral starvation impairs Paneth cell function, contributing to starvation-associated gut compromise.In this study, the effects of food deprivation on Paneth cell function were investigated using a mouse starvation model. We provide evidence that lack of enteral feeding results in Paneth cell autophagy, decreased expression of antimicrobial products (ie, lysozyme, cryptdin, and RegIII␥), and the presence of atypical secretory granules. Our results propose compromised Paneth cells to be involved in the reduced protection against bacterial translocation in enteral starvation.

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Secretion of microbicidal α-defensins by intestinal Paneth cells in response to bacteria

Cited by 960 publications

References 46 publications

NF-κB and the immune response

NF-κB and the immune response

Efficacy of Cryptdin-2 as an Adjunct to Antibiotics from Various Generations Against Salmonella

Starvation Compromises Paneth Cells

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