The Development of a Novel Multi-dimensional Product for Wound Healing Applications
A characteristic feature of chronic wounds is a prolonged inflammatory response as well as susceptibility to infection. Studies have shown that during the inflammatory response, there is a significant increase in the levels of neutrophil-derived enzymes. The purpose of this work was to determine whe...
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VCU Scholars Compass
2010
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ndltd-vcu.edu-oai-scholarscompass.vcu.edu-etd-31302017-03-17T08:33:09Z The Development of a Novel Multi-dimensional Product for Wound Healing Applications Roach, Necrisha A characteristic feature of chronic wounds is a prolonged inflammatory response as well as susceptibility to infection. Studies have shown that during the inflammatory response, there is a significant increase in the levels of neutrophil-derived enzymes. The purpose of this work was to determine whether the anionic macromolecule polystyrene sulfonate (PSS) and five of its salt forms, namely PSS-calcium, PSS-chlorhexidine, PSS-doxycycline, PSS-glutathione and PSS-silver are able to inhibit the activity of three of the enzymes whose levels are elevated in chronic wounds: elastase, cathepsin G and myeloperoxidase. In addition to the enzyme inhibition study, the various formulations’ antimicrobial properties were analyzed by evaluating their ability to inhibit the growth of three common clinical isolates: Staphylococcus aureus, Pseudomonas aeruginosa and Acinetobacter baumanii. It is worthy to note that the structure of PSS makes it a very flexible platform to which other molecules can be added in order to address a variety of “targets” as well as tailor quantitative strength. The results from this project showed that purified PSS and the various salt derivatives were able to inhibit elastase and cathepsin G activity. In addition, three of the therapeutic cations attached to PSS: silver, doxycycline and chlorhexidine retained their intrinsic antimicrobial properties without having an adverse effect on healthy tissue. In summary, this study demonstrated that PSS possessed an intrinsic ability to inhibit a number of proteases and that it could also be used as a delivery vehicle for other compounds with potential therapeutic value. 2010-05-05T07:00:00Z text application/pdf http://scholarscompass.vcu.edu/etd/2131 http://scholarscompass.vcu.edu/cgi/viewcontent.cgi?article=3130&context=etd © The Author Theses and Dissertations VCU Scholars Compass chronic wound myeloperoxidase polystyrene sulfonate elastase cathepsin G Life Sciences Physiology |
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chronic wound myeloperoxidase polystyrene sulfonate elastase cathepsin G Life Sciences Physiology |
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chronic wound myeloperoxidase polystyrene sulfonate elastase cathepsin G Life Sciences Physiology Roach, Necrisha The Development of a Novel Multi-dimensional Product for Wound Healing Applications |
| description |
A characteristic feature of chronic wounds is a prolonged inflammatory response as well as susceptibility to infection. Studies have shown that during the inflammatory response, there is a significant increase in the levels of neutrophil-derived enzymes. The purpose of this work was to determine whether the anionic macromolecule polystyrene sulfonate (PSS) and five of its salt forms, namely PSS-calcium, PSS-chlorhexidine, PSS-doxycycline, PSS-glutathione and PSS-silver are able to inhibit the activity of three of the enzymes whose levels are elevated in chronic wounds: elastase, cathepsin G and myeloperoxidase. In addition to the enzyme inhibition study, the various formulations’ antimicrobial properties were analyzed by evaluating their ability to inhibit the growth of three common clinical isolates: Staphylococcus aureus, Pseudomonas aeruginosa and Acinetobacter baumanii. It is worthy to note that the structure of PSS makes it a very flexible platform to which other molecules can be added in order to address a variety of “targets” as well as tailor quantitative strength. The results from this project showed that purified PSS and the various salt derivatives were able to inhibit elastase and cathepsin G activity. In addition, three of the therapeutic cations attached to PSS: silver, doxycycline and chlorhexidine retained their intrinsic antimicrobial properties without having an adverse effect on healthy tissue. In summary, this study demonstrated that PSS possessed an intrinsic ability to inhibit a number of proteases and that it could also be used as a delivery vehicle for other compounds with potential therapeutic value. |
| author |
Roach, Necrisha |
| author_facet |
Roach, Necrisha |
| author_sort |
Roach, Necrisha |
| title |
The Development of a Novel Multi-dimensional Product for Wound Healing Applications |
| title_short |
The Development of a Novel Multi-dimensional Product for Wound Healing Applications |
| title_full |
The Development of a Novel Multi-dimensional Product for Wound Healing Applications |
| title_fullStr |
The Development of a Novel Multi-dimensional Product for Wound Healing Applications |
| title_full_unstemmed |
The Development of a Novel Multi-dimensional Product for Wound Healing Applications |
| title_sort |
development of a novel multi-dimensional product for wound healing applications |
| publisher |
VCU Scholars Compass |
| publishDate |
2010 |
| url |
http://scholarscompass.vcu.edu/etd/2131 http://scholarscompass.vcu.edu/cgi/viewcontent.cgi?article=3130&context=etd |
| work_keys_str_mv |
AT roachnecrisha thedevelopmentofanovelmultidimensionalproductforwoundhealingapplications AT roachnecrisha developmentofanovelmultidimensionalproductforwoundhealingapplications |
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1718428988507947008 |