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MODELLING
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| - | + | <div align="center"><a href="https://2009.igem.org/Team:METU-Gene/Events_in_Wound_Dressing"><img src="https://static.igem.org/mediawiki/2009/d/d4/Events_in_WDk.gif" | |
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| + | title="Events in Wound Dressing"> | ||
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| + | title="Working Mechanism"> | ||
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| + | title="Methods and Results"> | ||
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| + | title="Modelling of Mechanism"> | ||
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| + | title="Focus on our Future!"></a></div></html> | ||
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| - | + | == Wound Dressing Mechanism == | |
| + | <html><div align="center" style="margin:15px 0px 0px 0px"><a href="https://2009.igem.org/2009.igem.org/metu-gene/parts"><img style="border: 0px solid ; width: 900px; height: 500px;" alt="w7" src="http://partsregistry.org/wiki/images/5/59/Mm.jpg"></a></div> | ||
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| + | ---- | ||
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| + | == Wound Dressing Layer Design == | ||
<div>Rapid and proper healing is important in the treatment of wounds such as severe burns, trauma, diabetic,decubitus and venous stasis ulcers, and similar tissue damages. In cases of severe and large amounts of skin loss, or in the presence of difficult and non-healing wounds, immediate coverage of the wound surface with a dressing is needed. The dressing achieves the functions of the natural skin by protecting the area from the loss of fluid and proteins, preventing infection through bacterial invasion, and subsequent tissue damage. In some cases, it improves healing by providing a support for the proliferating cells.</div> | <div>Rapid and proper healing is important in the treatment of wounds such as severe burns, trauma, diabetic,decubitus and venous stasis ulcers, and similar tissue damages. In cases of severe and large amounts of skin loss, or in the presence of difficult and non-healing wounds, immediate coverage of the wound surface with a dressing is needed. The dressing achieves the functions of the natural skin by protecting the area from the loss of fluid and proteins, preventing infection through bacterial invasion, and subsequent tissue damage. In some cases, it improves healing by providing a support for the proliferating cells.</div> | ||
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<a href="https://2009.igem.org/Team:METU-Gene/Biomaterial_Search"><img src="https://static.igem.org/mediawiki/2009/a/a1/Clgn.jpg" | <a href="https://2009.igem.org/Team:METU-Gene/Biomaterial_Search"><img src="https://static.igem.org/mediawiki/2009/a/a1/Clgn.jpg" | ||
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| + | == Biomaterials Modelling == | ||
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| - | < | + | <br>'''Characterization of the rhEGF-collagen sponges''' |
| - | <div | + | <div align="center">[1]'''Determination of the degree of crosslinking'''</div> |
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| - | The crosslinking degree could then be obtained from the differences between the absorbance values before and after | + | <br>The crosslinking degree could then be obtained from the differences between the absorbance values before and after |
the crosslinking. The equation is as follows: | the crosslinking. The equation is as follows: | ||
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where s is the sample and ncl is non-crosslinked. | where s is the sample and ncl is non-crosslinked. | ||
| - | < | + | <div align="center">[2]'''Water-binding capacity'''</div> |
| - | The water uptake of the collagen sponges was calculated using the following equation: | + | <br>The water uptake of the collagen sponges was calculated using the following equation: |
https://static.igem.org/mediawiki/2009/a/a3/Formul2.jpg | https://static.igem.org/mediawiki/2009/a/a3/Formul2.jpg | ||
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where Wd is the weight of the dry sponge and Ws is the weight of the swollen sponge. | where Wd is the weight of the dry sponge and Ws is the weight of the swollen sponge. | ||
| - | < | + | <div align="center">[3]'''Release kinetics'''</div> |
| - | To determine the possible release mechanism, drug release from collagen sponges was fitted to the following power model: | + | <br>To determine the possible release mechanism, drug release from collagen sponges was fitted to the following power model: |
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drug delivery system and n is the diffusional exponent which characterizes the drug transport mechanism. | drug delivery system and n is the diffusional exponent which characterizes the drug transport mechanism. | ||
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| + | <h2>Recombinant hEGF released from collagen sponges</h2> | ||
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| + | <p style="font-size:110%; color:#576f91; font-family:georgia,serif;"><br>Figure 1 shows the release profiles of rhEGF from collagen sponge at 37 �C in PBS with/without collagenase solution. | ||
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| + | Chih-Hui Yang in his study supposed that under the in vitro non-degradation conditions, rhEGF was initially released by diffusion. Generally speaking, since collagen is enzymatically degraded, low final release values are expected in the absence of any enzymes. Therefore, collagenase was employed for the model of the in vitro rhEGF release study. In project, this case is also valuable. | ||
| - | + | <br>Therefore, the influence of the types and the concentrations of the crosslinking agents and the preparation conditions on the structures and characteristics of collagen sponges, and the rhEGF release from collagen sponges were compared in his study.</p> | |
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| - | < | + | <h2>The rhEGF release patterns from collagen sponges </h2> |
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| + | <p style="font-size:110%; color:#576f91; font-family:georgia,serif;"><br><br>Three different types of crosslinking agents, GTA, genipin and ECD were used to prepare crosslinked collagen sponges. The rhEGF release patterns from collagen sponges are shown in Figure 2. | ||
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The drug release rate from crosslinked collagen sponges treated with EDC was the fastest, followed by collagen sponges treated with genipin and GTA, respectively. The EDC crosslinked collagen showed no release control effect, | The drug release rate from crosslinked collagen sponges treated with EDC was the fastest, followed by collagen sponges treated with genipin and GTA, respectively. The EDC crosslinked collagen showed no release control effect, | ||
which was probably due to the fact that EDC increased the water-solubility and lowered the viscosity of collagen (data | which was probably due to the fact that EDC increased the water-solubility and lowered the viscosity of collagen (data | ||
| - | not shown). GTA crosslinked collagen showed the most potent release control effect than the other two (EDC and genipin). '''However, since we want controlled and orderly release system which will be improved our transgenic bacteria, we used genipin for formation our cellulose Wound Dressing layer in three different types of crosslinking agents, GTA, genipin and ECD.''' | + | not shown). GTA crosslinked collagen showed the most potent release control effect than the other two (EDC and genipin). '''However, since we want controlled and orderly release system which will be improved our transgenic bacteria, we used genipin for formation our cellulose Wound Dressing layer in three different types of crosslinking agents, GTA, genipin and ECD.'''</p> |
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Latest revision as of 22:45, 21 October 2009
Contents |
Wound Dressing Mechanism
Wound Dressing Layer Design
Rapid and proper healing is important in the treatment of wounds such as severe burns, trauma, diabetic,decubitus and venous stasis ulcers, and similar tissue damages. In cases of severe and large amounts of skin loss, or in the presence of difficult and non-healing wounds, immediate coverage of the wound surface with a dressing is needed. The dressing achieves the functions of the natural skin by protecting the area from the loss of fluid and proteins, preventing infection through bacterial invasion, and subsequent tissue damage. In some cases, it improves healing by providing a support for the proliferating cells.
