Abstract

Human β-defensins (hBDs) are small, cationic antimicrobial peptides, secreted by mucosal epithelial cells that regulate adaptive immune functions. We previously reported that Fusobacterium nucleatum, a ubiquitous gram-negative bacterium of the human oral cavity, induces human β-defensin 2 (hBD2) upon contact with primary oral epithelial cells. We now report the isolation and characterization of an F. nucleatum (ATCC 25586)-associated defensin inducer (FAD-I). Biochemical approaches revealed a cell wall fraction containing four proteins that stimulated the production of hBD2 in human oral epithelial cells (HOECs). Cross-referencing of the N-terminal sequences of these proteins with the F. nucleatum genome revealed that the genes encoding the proteins were FadA, FN1527, FN1529, and FN1792. Quantitative PCR of HOEC monolayers challenged with Escherichia coli clones expressing the respective cell wall proteins revealed that FN1527 was most active in the induction of hBD2 and hence was termed FAD-I. We tagged FN1527 with a c-myc epitope on the C-terminal end to identify and purify it from the E. coli clone. Purified FN1527 (FAD-I) induced hBD2 mRNA and protein expression in HOEC monolayers. F. nucleatum cell wall and FAD-I induced hBD2 via TLR2. Porphorymonas gingivalis, an oral pathogen that does not induce hBD2 in HOECs, was able to significantly induce expression of hBD2 in HOECs only when transformed to express FAD-I. FAD-I or its derivates offer a potentially new paradigm in immunoregulatory therapeutics because they may one day be used to bolster the innate defenses of vulnerable mucosae.

Highlights

  • Oral mucosal epithelium represents the first line of defense against invading microbes

  • By expressing FN1527 in Porphyromonas gingivalis, an opportunistic Gram-negative bacterium strongly implicated in periodontal disease and an organism that does not induce appreciable levels of hBD mRNA in human oral epithelial cells (HOECs) when compared with F. nucleatum [17], we were able to show that the transformed bacterium could induce hBD2 significantly more than the parent strain

  • The chemokine IL-8 was not induced by Fusobacterium-associated defensin inducer (FAD-I) in these cells, contrary to what we and others have reported for F. nucleatum whole bacteria and its cell wall fraction [17, 29, 30, 32,33,34]

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Summary

EXPERIMENTAL PROCEDURES

Healthy oral tissue overlying impacted third molars of normal adults were extracted and used to isolate HOECs, as NOVEMBER 19, 2010 VOLUME 285 NUMBER 47

FadA Hypothetical Hypothetical Hypothetical
Primer sequence
RESULTS
DISCUSSION
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