4.2 Article

Multispecific myeloid defensins

Journal

CURRENT OPINION IN HEMATOLOGY
Volume 14, Issue 1, Pages 16-21

Publisher

LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1097/00062752-200701000-00005

Keywords

antiviral; defensins; retrocyclins; toxin-neutralizing

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Purpose of review This review describes recent progress in our understanding of defensins and their contributions to innate immunity. Defensins are small, cysteine-rich endogenous antibiotic peptides. Human neutrophils contain large amounts of three alpha-defensins (HNP-1-HNP-3), and smaller amounts of a fourth, HNP-4. Monocytes and macrophages generally lack defensins, but they release messengers that induce the synthesis of beta-defensins in epithelial cells. Recent findings In addition to their antimicrobial and immunomodulatory effects, HNP-1-HNP-3 possess antiviral and toxin-neutralizing properties. Induction of beta-defensins in epithelial cells is mediated by cell-surface Toll-like receptors or cytoplasmic peptidoglycan receptors that can recognize pathogen-associated molecules. Mutations in Nod2, a cytoplasmic peptidoglycan receptor, are associated with reduced levels of intestinal alpha-defensins and ileal Crohn's disease. Human defensin genes show marked copy-number polymorphism. High level constitutive expression of defensins may afford protection against HIV-1 and other defensin-sensitive pathogens. Theta-defensins (cyclic octadecapeptides found in nonhuman primates) have impressive antiviral and antitoxic properties. Summary The multiple properties of defensins contribute to human innate immunity against bacteria, bacteria] toxins, and viruses.

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