Human β-defensin 4 – defensin without the “twist”

Authors

  • Adam Prahl Faculty of Chemistry, Department of Organic Chemistry, University of Gdansk, Gdansk, Poland
  • Marzena Pazgier Division of Vaccine Research, Institute of Hu - man Virology, University of Maryland School of Medicine, Baltimore, MD, USA
  • Jerry Alexandratos Macromolecular Crystallography Laboratory, Center for Cancer Research, National Cancer Institute, Frederick MD, USA
  • Jacek Lubkowski Macromolecular Crystallography Laboratory, Center for Cancer Research, National Cancer Institute, Frederick MD, USA

DOI:

https://doi.org/10.18388/pb.2016_36

Abstract

β-defensins are small, cysteine-rich, cationic peptides that contribute to various processes related to both arms of host defense, the innate and adaptive immunities. All β-defensins are potent antimicrobials with activity targeting a broad range of pathogens. Some human β-defensins (hBDs) are also capable of binding and activating specific chemokine receptors, leading to chemotaxis of receptor-presenting cells. Two receptors identified as targets of specific human β-defensins are CCR2 and CCR6, both members of the seven-transmembrane family of chemokine receptors. Currently, around 50 open reading frames (ORFs) identified in the human genome encode proteins that have signatures characteristic of β-defensins. Of those, only three, hBD1-3, have been thoroughly characterized to date, including a detailed structural description of their molecules. In addition, limited information on biological and bactericidal properties is available for hBD4, as well as the solution structure of hBD6. The crystal structure of hBD4, determined here at resolution of 1.60 Å, indicates significant structural differences between this molecule and those reported previously for other hBDs. Crystallographic studies indicate a possibility of unique dimerization of hBD4, confirmed by solution studies using analytical ultracentrifugation. In contrast to hBD1-3, hBD4 does not induce CCR6-mediated chemotaxis. This observation can be attributed to an unusual conformation of the hBD4 N-terminus. In agreement with previously published reports, hBD4 was shown to be a potent antibacterial agent, as demonstrated by results of assays with E. coli ATCC 25922 cells.

Downloads

Download data is not yet available.
Cover 3 2016

Downloads

Published

2016-11-15

Issue

Vol. 62 No. 3 (2016): Alexander Wlodawer 70th Birthday

Section

Articles

License

All journal contents are distributed under the Creative Commons Attribution-ShareAlike 4.0 International (CC BY-SA 4.0) license. Everybody may use the content following terms: Attribution — You must give appropriate credit, provide a link to the license, and indicate if changes were made, ShareAlike — If you remix, transform, or build upon the material, you must distribute your contributions under the same license as the original. There are no additional restrictions — You may not apply legal terms or technological measures that legally restrict others from doing anything the license permits.

Copyright for all published papers © stays with the authors.

Copyright for the journal: © Polish Biochemical Society.