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Topical and local controlled release of stratifin for the improvement of hypertrophic scarring in open and surgically closed wounds Rahmani Neishaboor, Elham
Abstract
Hypertrophic scar (HS), which results from the uncontrolled synthesis and excessive deposition of extracellular matrix (ECM) at sites of dermal injury, represents an undesirable endpoint of wound healing. Stratifin (SFN) was recently identified as a potent matrix methaloproteinase-1 (MMP-1) stimulatory factor in dermal fibroblasts. In this research project, it is hypothesized that stratifin can modulate the deposition of ECM components and prevent HS formation when it is applied topically to open wounds or locally delivered to surgically closed wounds. Four specific objectives were accomplished in this project. Under objective 1, a hydrogel /microsphere dermal implant was fabricated, specifically to be placed in surgical wounds before closure and locally deliver stratifin in a controlled manner to reduce HS formation. Microencapsulating stratifin complexed chitosan particles into PLGA microspheres allowed bioactive stratifin to be controllably released over 30 days with a reduced burst release. Under objective 2, use of a rat surgical wound model showed that the local controlled delivery of stratifin markedly reduced fibrosis and inflammation induced by drug-free implants, confirmed by a reduced collagen deposition, total tissue cellularity, and infiltrated CDHypertrophic scar (HS), which results from the uncontrolled synthesis and excessive deposition of extracellular matrix (ECM) at sites of dermal injury, represents an undesirable endpoint of wound healing. Stratifin (SFN) was recently identified as a potent matrix methaloproteinase-1 (MMP-1) stimulatory factor in dermal fibroblasts. In this research project, it is hypothesized that stratifin can modulate the deposition of ECM components and prevent HS formation when it is applied topically to open wounds or locally delivered to surgically closed wounds. Four specific objectives were accomplished in this project. Under objective 1, a hydrogel /microsphere dermal implant was fabricated, specifically to be placed in surgical wounds before closure and locally deliver stratifin in a controlled manner to reduce HS formation. Microencapsulating stratifin complexed chitosan particles into PLGA microspheres allowed bioactive stratifin to be controllably released over 30 days with a reduced burst release. Under objective 2, use of a rat surgical wound model showed that the local controlled delivery of stratifin markedly reduced fibrosis and inflammation induced by drug-free implants, confirmed by a reduced collagen deposition, total tissue cellularity, and infiltrated CD³⁺ immune cells. Under objective 3, the anti-fibrogenic effect of topically applied stratifin was investigated on open wounds created in a rabbit ear fibrotic model. Qualitative wound assessment showed a reduced HS in wounds treated with stratifin-impregnated CMC gel (0.002%, w/w) applied twice a day, confirmed with reduced scar volume including deposited collagen and total tissue cellularity. Under objective 4, CMC gel was modified into a thermoreversible emulgel, which demonstrated a significant effect on scar reduction through its occlusive effect. Using this emulgel and combining stratifin with acetylsalicylic acid significantly reduced HS, even with once a day application. In conclusion, the findings presented in this thesis provide further support for the importance and feasibility of using stratifin as an MMP-1 stimulatory factor for the improvement/prevention of dermal fibrosis in open and surgically closed wounds. These findings also provide additional information regarding controlled delivery of proteins to any kind of wounds, such as those resulting from surgical or burns. immune cells. Under objective 3, the anti-fibrogenic effect of topically applied stratifin was investigated on open wounds created in a rabbit ear fibrotic model. Qualitative wound assessment showed a reduced HS in wounds treated with stratifin-impregnated CMC gel (0.002%, w/w) applied twice a day, confirmed with reduced scar volume including deposited collagen and total tissue cellularity. Under objective 4, CMC gel was modified into a thermoreversible emulgel, which demonstrated a significant effect on scar reduction through its occlusive effect. Using this emulgel and combining stratifin with acetylsalicylic acid significantly reduced HS, even with once a day application. In conclusion, the findings presented in this thesis provide further support for the importance and feasibility of using stratifin as an MMP-1 stimulatory factor for the improvement/prevention of dermal fibrosis in open and surgically closed wounds. These findings also provide additional information regarding controlled delivery of proteins to any kind of wounds, such as those resulting from surgical or burns.
Item Metadata
Title |
Topical and local controlled release of stratifin for the improvement of hypertrophic scarring in open and surgically closed wounds
|
Creator | |
Publisher |
University of British Columbia
|
Date Issued |
2011
|
Description |
Hypertrophic scar (HS), which results from the uncontrolled synthesis and
excessive deposition of extracellular matrix (ECM) at sites of dermal injury, represents
an undesirable endpoint of wound healing. Stratifin (SFN) was recently identified as a
potent matrix methaloproteinase-1 (MMP-1) stimulatory factor in dermal fibroblasts. In
this research project, it is hypothesized that stratifin can modulate the deposition of ECM
components and prevent HS formation when it is applied topically to open wounds or
locally delivered to surgically closed wounds.
Four specific objectives were accomplished in this project. Under objective 1, a
hydrogel /microsphere dermal implant was fabricated, specifically to be placed in
surgical wounds before closure and locally deliver stratifin in a controlled manner to
reduce HS formation. Microencapsulating stratifin complexed chitosan particles into
PLGA microspheres allowed bioactive stratifin to be controllably released over 30 days
with a reduced burst release. Under objective 2, use of a rat surgical wound model
showed that the local controlled delivery of stratifin markedly reduced fibrosis and
inflammation induced by drug-free implants, confirmed by a reduced collagen deposition,
total tissue cellularity, and infiltrated CDHypertrophic scar (HS), which results from the uncontrolled synthesis and
excessive deposition of extracellular matrix (ECM) at sites of dermal injury, represents
an undesirable endpoint of wound healing. Stratifin (SFN) was recently identified as a
potent matrix methaloproteinase-1 (MMP-1) stimulatory factor in dermal fibroblasts. In
this research project, it is hypothesized that stratifin can modulate the deposition of ECM
components and prevent HS formation when it is applied topically to open wounds or
locally delivered to surgically closed wounds.
Four specific objectives were accomplished in this project. Under objective 1, a
hydrogel /microsphere dermal implant was fabricated, specifically to be placed in
surgical wounds before closure and locally deliver stratifin in a controlled manner to
reduce HS formation. Microencapsulating stratifin complexed chitosan particles into
PLGA microspheres allowed bioactive stratifin to be controllably released over 30 days
with a reduced burst release. Under objective 2, use of a rat surgical wound model
showed that the local controlled delivery of stratifin markedly reduced fibrosis and
inflammation induced by drug-free implants, confirmed by a reduced collagen deposition,
total tissue cellularity, and infiltrated CD³⁺ immune cells.
Under objective 3, the anti-fibrogenic effect of topically applied stratifin was
investigated on open wounds created in a rabbit ear fibrotic model. Qualitative wound
assessment showed a reduced HS in wounds treated with stratifin-impregnated CMC gel
(0.002%, w/w) applied twice a day, confirmed with reduced scar volume including
deposited collagen and total tissue cellularity. Under objective 4, CMC gel was modified
into a thermoreversible emulgel, which demonstrated a significant effect on scar
reduction through its occlusive effect. Using this emulgel and combining stratifin with
acetylsalicylic acid significantly reduced HS, even with once a day application.
In conclusion, the findings presented in this thesis provide further support for the
importance and feasibility of using stratifin as an MMP-1 stimulatory factor for the
improvement/prevention of dermal fibrosis in open and surgically closed wounds. These
findings also provide additional information regarding controlled delivery of proteins to
any kind of wounds, such as those resulting from surgical or burns. immune cells.
Under objective 3, the anti-fibrogenic effect of topically applied stratifin was
investigated on open wounds created in a rabbit ear fibrotic model. Qualitative wound
assessment showed a reduced HS in wounds treated with stratifin-impregnated CMC gel
(0.002%, w/w) applied twice a day, confirmed with reduced scar volume including
deposited collagen and total tissue cellularity. Under objective 4, CMC gel was modified
into a thermoreversible emulgel, which demonstrated a significant effect on scar
reduction through its occlusive effect. Using this emulgel and combining stratifin with
acetylsalicylic acid significantly reduced HS, even with once a day application.
In conclusion, the findings presented in this thesis provide further support for the
importance and feasibility of using stratifin as an MMP-1 stimulatory factor for the
improvement/prevention of dermal fibrosis in open and surgically closed wounds. These
findings also provide additional information regarding controlled delivery of proteins to
any kind of wounds, such as those resulting from surgical or burns.
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Genre | |
Type | |
Language |
eng
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Date Available |
2011-08-31
|
Provider |
Vancouver : University of British Columbia Library
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Rights |
Attribution-NonCommercial-NoDerivatives 4.0 International
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DOI |
10.14288/1.0071610
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URI | |
Degree | |
Program | |
Affiliation | |
Degree Grantor |
University of British Columbia
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Graduation Date |
2011-05
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Campus | |
Scholarly Level |
Graduate
|
Rights URI | |
Aggregated Source Repository |
DSpace
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Rights
Attribution-NonCommercial-NoDerivatives 4.0 International