4.4 Article

Differential regulation of human cathelicidin LL-37 by free fatty acids and their analogs

Journal

PEPTIDES
Volume 50, Issue -, Pages 129-138

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.peptides.2013.10.008

Keywords

LL-37; Host defense peptides; Cathelicidins; Short-chain fatty acids; Butyrate; Hexanoate; Heptanoate

Funding

  1. USDA/NIFA [2008-35204-04-544]
  2. Oklahoma Center for the Advancement of Science and Technology [AR12.2-077, HR12-051]
  3. Oklahoma State University Technology Business Development Program grant
  4. Oklahoma Agricultural Experiment Station [H-2811]

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LL-37 is the single cathelicidin host defense peptide in humans with direct antimicrobial and immunomodulatory activities. Specific regulation of LL-37 synthesis has emerged as a novel non-antibiotic approach to disease control and prevention. Short-chain fatty acids, and butyrate in particular, were found recently to be strong inducers of LL-37 gene expression without causing inflammation. Here, we further evaluated the LL-37-inducing efficiency of a broad range of saturated free fatty acids and their derivatives in human HT-29 colonic epithelial cells and U-937 monocytic cells by real-time RT-PCR. Surprisingly, we revealed that valerate, hexanoate, and heptanoate with 5-7 carbons are more potent than 4-carbon butyrate in promoting LL-37 gene expression in both cell types. Free fatty acids with longer than 7 or shorter than 4 carbons showed only a marginal effect on LL-37 expression. Studies with a series of fatty acid derivatives with modifications in the aliphatic chain or carboxylic acid group yielded several analogs such as benzyl butyrate, trans-cinnamyl butyrate, glyceryl tributyrate, and phenethyl butyrate with a comparable LL-37-inducing activity to sodium butyrate. On the other hand, although reactive, the anhydride derivatives of short-and medium-chain fatty acids are as potent as their corresponding free acid forms in LL-37 induction. Thus, these newly identified free fatty acids and their analogs with a strong capacity to augment LL-37 synthesis may hold promise as immune boosting dietary supplements for antimicrobial therapy. (C) 2013 Elsevier Inc. All rights reserved.

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