In vivo efficacy of novel antibacterial and immunomodulatory peptides

In vivo efficacy of novel antibacterial and immunomodulatory peptides

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Despite the success of modern medicine in treating infections, infectious diseases remain a major source of morbidity and mortality worldwide. The evolution of antibiotic resistant strains of bacteria means that new innovations in therapeutics must be pursued to combat this emerging threat. A novel...

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Main Author: Waldbrook, Matthew George
Format: Others
Language:English
Published: University of British Columbia 2008
Subjects:
Antimicrobial peptides
Immunomodulation
Mouse model
Alternate antibiotics
Online Access:http://hdl.handle.net/2429/2850
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spelling ndltd-UBC-oai-circle.library.ubc.ca-2429-28502018-01-05T17:23:09Z In vivo efficacy of novel antibacterial and immunomodulatory peptides Waldbrook, Matthew George Antimicrobial peptides Immunomodulation Mouse model Alternate antibiotics Despite the success of modern medicine in treating infections, infectious diseases remain a major source of morbidity and mortality worldwide. The evolution of antibiotic resistant strains of bacteria means that new innovations in therapeutics must be pursued to combat this emerging threat. A novel approach is to utilize the anti-infective properties of endogenous host defense peptides by creating smaller synthetic peptides with enhanced protective activities. Some of these peptides directly kill bacteria and many display varied immunomodulatory activities, enhancing the host innate immune response to more effectively clear an infection. Here I examined the efficacy of several synthetic peptides in a murine model of invasive bacterial infection, induced by the Gram positive bacterium Staphylococcus aureus. Several peptides were able to significantly reduce peritoneal bacterial load in vivo by up to 4-logs relative to the controls, either through direct antibacterial killing or immunomodulatory activity. The latter class was studied in more detail; in particular, the peptides IDR-1 and 1002 displayed significant immunomodulatory effects in vivo. Both peptides were able to significantly induce the proinflammatory chemokines MCP-1, RANTES and KC, as well as increased recruitment of neutrophils and monocytes to the site of infection. These effects were not dependent on live bacteria, as heat inactivated S. aureus was also able to induce chemokines and cell migration. Mice that had been depleted of macrophages did not respond to peptide treatment, indicating that macrophages are an important effector cells through which immunomodulatory peptides counter infections. These results suggest that synthetic peptides have the potential to become a viable treatment option for bacterial infections. Science, Faculty of Microbiology and Immunology, Department of Graduate 2008-12-08T16:53:45Z 2008-12-08T16:53:45Z 2008 2009-05 Text Thesis/Dissertation http://hdl.handle.net/2429/2850 eng Attribution-NonCommercial-NoDerivatives 4.0 International http://creativecommons.org/licenses/by-nc-nd/4.0/ 1621611 bytes application/pdf University of British Columbia
collection NDLTD
language English
format Others
sources NDLTD
topic Antimicrobial peptides
Immunomodulation
Mouse model
Alternate antibiotics
spellingShingle Antimicrobial peptides
Immunomodulation
Mouse model
Alternate antibiotics
Waldbrook, Matthew George
In vivo efficacy of novel antibacterial and immunomodulatory peptides
description Despite the success of modern medicine in treating infections, infectious diseases remain a major source of morbidity and mortality worldwide. The evolution of antibiotic resistant strains of bacteria means that new innovations in therapeutics must be pursued to combat this emerging threat. A novel approach is to utilize the anti-infective properties of endogenous host defense peptides by creating smaller synthetic peptides with enhanced protective activities. Some of these peptides directly kill bacteria and many display varied immunomodulatory activities, enhancing the host innate immune response to more effectively clear an infection. Here I examined the efficacy of several synthetic peptides in a murine model of invasive bacterial infection, induced by the Gram positive bacterium Staphylococcus aureus. Several peptides were able to significantly reduce peritoneal bacterial load in vivo by up to 4-logs relative to the controls, either through direct antibacterial killing or immunomodulatory activity. The latter class was studied in more detail; in particular, the peptides IDR-1 and 1002 displayed significant immunomodulatory effects in vivo. Both peptides were able to significantly induce the proinflammatory chemokines MCP-1, RANTES and KC, as well as increased recruitment of neutrophils and monocytes to the site of infection. These effects were not dependent on live bacteria, as heat inactivated S. aureus was also able to induce chemokines and cell migration. Mice that had been depleted of macrophages did not respond to peptide treatment, indicating that macrophages are an important effector cells through which immunomodulatory peptides counter infections. These results suggest that synthetic peptides have the potential to become a viable treatment option for bacterial infections. === Science, Faculty of === Microbiology and Immunology, Department of === Graduate
author Waldbrook, Matthew George
author_facet Waldbrook, Matthew George
author_sort Waldbrook, Matthew George
title In vivo efficacy of novel antibacterial and immunomodulatory peptides
title_short In vivo efficacy of novel antibacterial and immunomodulatory peptides
title_full In vivo efficacy of novel antibacterial and immunomodulatory peptides
title_fullStr In vivo efficacy of novel antibacterial and immunomodulatory peptides
title_full_unstemmed In vivo efficacy of novel antibacterial and immunomodulatory peptides
title_sort in vivo efficacy of novel antibacterial and immunomodulatory peptides
publisher University of British Columbia
publishDate 2008
url http://hdl.handle.net/2429/2850
work_keys_str_mv AT waldbrookmatthewgeorge invivoefficacyofnovelantibacterialandimmunomodulatorypeptides
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