Paneth cell trypsin is the processing enzyme for human defensin-5

Ghosh, Dipankar; Porter, Edith; Shen, Bo; Lee, Sarah K.; Wilk, Dennis; Drazba, Judith A.; Yadav, Satya Prakash; Crabb, John W.; Ganz, Tomas; Bevins, Charles L.

doi:10.1038/ni797

Cited by 391 publications

(392 citation statements)

References 61 publications

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“…In Paneth cells, this processing is accomplished by tryptic digestion during or just after secretion into the intestinal lumen (55). A recent report has shown that, in the male urethra, HD-5 processing may depend on proteases secreted by neutrophils (50).…”

Section: Discussionmentioning

confidence: 99%

Human α-defensins block papillomavirus infection

Buck

Day

Thompson

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

213

169

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Section: Discussionmentioning

confidence: 99%

Human α-defensins block papillomavirus infection

Buck

Day

Thompson

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

213

169

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“…Protein extracts from ileal mucosa were isolated from randomly selected controls, CD NOD2͞CARD15 wild-type and CD NOD2͞CARD15 SNP13 patients, as described (35). Protein expression of HD5, ␣-1-trypsin inhibitor, lysozyme, and sPLA 2 in the patient samples was quantified by immunoblotting, as described (36).…”

Section: Methodsmentioning

confidence: 99%

“…Cationic proteins from ileal mucosal biopsies were isolated by using a weak cation exchange matrix, as described (35). Assays were normalized to protein concentration, as determined by Bradford assay.…”

Section: Methodsmentioning

confidence: 99%

Reduced Paneth cell α-defensins in ileal Crohn's disease

Wehkamp

Salzman

Porter

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

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890

807

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The pathogenesis of Crohn s disease (CD), an idiopathic inflammatory bowel disease, is attributed, in part, to intestinal bacteria that may initiate and perpetuate mucosal inflammation in genetically susceptible individuals. Paneth cells (PC) are the major source of antimicrobial peptides in the small intestine, including human ␣-defensins HD5 and HD6. We tested the hypothesis that reduced expression of PC ␣-defensins compromises mucosal host defenses and predisposes patients to CD of the ileum. We report that patients with CD of the ileum have reduced antibacterial activity in their intestinal mucosal extracts. These specimens also showed decreased expression of PC ␣-defensins, whereas the expression of eight other PC products either remained unchanged or increased when compared with controls. The specific decrease of ␣-defensins was independent of the degree of inflammation in the specimens and was not observed in either CD of the colon, ulcerative colitis, or pouchitis. The functional consequence of ␣-defensin expression levels was examined by using a transgenic mouse model, where we found changes in HD5 expression levels, comparable to those observed in CD, had a pronounced impact on the luminal microbiota. Thus, the specific deficiency of PC defensins that characterizes ileal CD may compromise innate immune defenses of the ileal mucosa and initiate and͞or perpetuate this disease.innate immunity ͉ intestine ͉ bacteria ͉ inflammatory bowel disease

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“…In humans, six members of the ␣-defensin family have been described: human neutrophil peptides 1-4 (HNP1 to -4) present in the neutrophil granules (19 -22) and human defensin 5 and 6 (HD5 and -6) secreted by the Paneth cells of the intestinal crypts (23,24). Each of the six ␣-defensins is expressed with a pro-domain, which functions in sorting to the correct compartment, the inhibition of activity while the pro-peptide is still attached, and the facilitation of the correct folding of the mature defensin (25)(26)(27)(28)(29)(30)(31).…”

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confidence: 99%

“…Collectively, these studies have provided important insights into the structural and functional roles of disulfide bonding (51,52), cationicity (53,54), and conserved elements, such as the Arg-Glu salt bridge (55)(56)(57)(58) and invariant Gly residue (59,60) in the action of ␣-defensins. Recently, a comprehensive Ala scanning mutagenesis of HNP1 has discovered that a hydrophobic residue near the C terminus, Trp 26 , governs the ability of this ␣-defensin to kill Staphylococcus aureus, inhibit anthrax lethal factor, and bind HIV-1 envelope glycoprotein gp120 (61); methylation of a peptide bond at the putative dimer interface of HNP1 debilitates its dimerization and is functionally detrimental (62). Despite structural conservation, mammalian ␣-defensins share rather limited sequence identity.…”

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confidence: 99%

Functional Determinants of Human Enteric α-Defensin HD5

Rajabi

Ericksen

et al. 2012

Journal of Biological Chemistry

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Background: Human ␣-defensin HD5 is a multifunctional antimicrobial peptide whose functional determinants have yet to be elucidated. Results: Alanine scanning mutagenesis aided by x-ray crystallography identified Leu 29 at the dimer interface as crucial; N-methylation of Glu 21 to debilitate HD5 dimerization also affected activity. Conclusion: Dimerization and hydrophobicity are important for HD5 function. Significance: The molecular basis of ␣-defensin function is better understood.

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Paneth cell trypsin is the processing enzyme for human defensin-5

Cited by 391 publications

References 61 publications

Human α-defensins block papillomavirus infection

Human α-defensins block papillomavirus infection

Reduced Paneth cell α-defensins in ileal Crohn's disease

Functional Determinants of Human Enteric α-Defensin HD5

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