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A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity

A novel defensin antimicrobial peptide gene was identified in Atlantic cod, Gadus morhua. This three exon/two intron defensin gene codes for a peptide precursor consisting of two domains: a signal peptide of 26 amino acids and a mature peptide of 40 residues. The mature cod defensin has six conserve...

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Autores principales: Ruangsri, Jareeporn, Kitani, Yoichiro, Kiron, Viswanath, Lokesh, Jep, Brinchmann, Monica F., Karlsen, Bård Ove, Fernandes, Jorge M. O.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3636224/
https://www.ncbi.nlm.nih.gov/pubmed/23638029
http://dx.doi.org/10.1371/journal.pone.0062302
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author Ruangsri, Jareeporn
Kitani, Yoichiro
Kiron, Viswanath
Lokesh, Jep
Brinchmann, Monica F.
Karlsen, Bård Ove
Fernandes, Jorge M. O.
author_facet Ruangsri, Jareeporn
Kitani, Yoichiro
Kiron, Viswanath
Lokesh, Jep
Brinchmann, Monica F.
Karlsen, Bård Ove
Fernandes, Jorge M. O.
author_sort Ruangsri, Jareeporn
collection PubMed
description A novel defensin antimicrobial peptide gene was identified in Atlantic cod, Gadus morhua. This three exon/two intron defensin gene codes for a peptide precursor consisting of two domains: a signal peptide of 26 amino acids and a mature peptide of 40 residues. The mature cod defensin has six conserved cysteine residues that form 1–5, 2–4 and 3–6 disulphide bridges. This pattern is typical of beta-defensins and this gene was therefore named cod beta-defensin (defb). The tertiary structure of Defb exhibits an α/β fold with one α helix and β(1)β(2)β(3) sheets(.) RT-PCR analysis indicated that defb transcripts were present mainly in the swim bladder and peritoneum wall but could also be detected at moderate to low levels in skin, head- and excretory kidneys. In situ hybridisation revealed that defb was specifically expressed by cells located in the swim bladder submucosa and the oocytes. During embryonic development, defb gene transcripts were detectable from the golden eye stage onwards and their expression was restricted to the swim bladder and retina. Defb was differentially expressed in several tissues following antigenic challenge with Vibrio anguillarum, being up-regulated up to 25-fold in head kidney. Recombinant Defb displayed antibacterial activity, with a minimal inhibitory concentration of 0.4–0.8 µM and 25–50 µM against the Gram-(+) bacteria Planococcus citreus and Micrococcus luteus, respectively. In addition, Defb stimulated phagocytic activity of cod head kidney leucocytes in vitro. These findings imply that beta-defensins may play an important role in the innate immune response of Atlantic cod.
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spelling pubmed-36362242013-05-01 A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity Ruangsri, Jareeporn Kitani, Yoichiro Kiron, Viswanath Lokesh, Jep Brinchmann, Monica F. Karlsen, Bård Ove Fernandes, Jorge M. O. PLoS One Research Article A novel defensin antimicrobial peptide gene was identified in Atlantic cod, Gadus morhua. This three exon/two intron defensin gene codes for a peptide precursor consisting of two domains: a signal peptide of 26 amino acids and a mature peptide of 40 residues. The mature cod defensin has six conserved cysteine residues that form 1–5, 2–4 and 3–6 disulphide bridges. This pattern is typical of beta-defensins and this gene was therefore named cod beta-defensin (defb). The tertiary structure of Defb exhibits an α/β fold with one α helix and β(1)β(2)β(3) sheets(.) RT-PCR analysis indicated that defb transcripts were present mainly in the swim bladder and peritoneum wall but could also be detected at moderate to low levels in skin, head- and excretory kidneys. In situ hybridisation revealed that defb was specifically expressed by cells located in the swim bladder submucosa and the oocytes. During embryonic development, defb gene transcripts were detectable from the golden eye stage onwards and their expression was restricted to the swim bladder and retina. Defb was differentially expressed in several tissues following antigenic challenge with Vibrio anguillarum, being up-regulated up to 25-fold in head kidney. Recombinant Defb displayed antibacterial activity, with a minimal inhibitory concentration of 0.4–0.8 µM and 25–50 µM against the Gram-(+) bacteria Planococcus citreus and Micrococcus luteus, respectively. In addition, Defb stimulated phagocytic activity of cod head kidney leucocytes in vitro. These findings imply that beta-defensins may play an important role in the innate immune response of Atlantic cod. Public Library of Science 2013-04-25 /pmc/articles/PMC3636224/ /pubmed/23638029 http://dx.doi.org/10.1371/journal.pone.0062302 Text en © 2013 Ruangsri et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Ruangsri, Jareeporn
Kitani, Yoichiro
Kiron, Viswanath
Lokesh, Jep
Brinchmann, Monica F.
Karlsen, Bård Ove
Fernandes, Jorge M. O.
A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity
title A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity
title_full A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity
title_fullStr A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity
title_full_unstemmed A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity
title_short A Novel Beta-Defensin Antimicrobial Peptide in Atlantic Cod with Stimulatory Effect on Phagocytic Activity
title_sort novel beta-defensin antimicrobial peptide in atlantic cod with stimulatory effect on phagocytic activity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3636224/
https://www.ncbi.nlm.nih.gov/pubmed/23638029
http://dx.doi.org/10.1371/journal.pone.0062302
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