Difference between revisions of "Team:Queens Canada/Description"
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<h2>Icefinity</h2> | <h2>Icefinity</h2> | ||
<p>As an addition to our project this year, we decided to further explore the topic of AFPs and their variety of applications. Protein stability is of great importance when considering the use of AFPs in industry. Typical industrial processes often involve harsh conditions which will lead to denaturation (i.e. loss of function) for the protein. Therefore, in conjunction with improving the activity of the Type III AFP, we set out to increase the stability of the protein through circularization techniques.</p> | <p>As an addition to our project this year, we decided to further explore the topic of AFPs and their variety of applications. Protein stability is of great importance when considering the use of AFPs in industry. Typical industrial processes often involve harsh conditions which will lead to denaturation (i.e. loss of function) for the protein. Therefore, in conjunction with improving the activity of the Type III AFP, we set out to increase the stability of the protein through circularization techniques.</p> | ||
− | <p>Using Heidelberg’s intein biobrick <a href="http://parts.igem.org/Part:BBa_K1362000">BBa_K1362000</a>, we performed the intein-splicing reaction with the AFP to generate a circular protein: Icefinity. Heidelberg and other research parties have shown an increase in thermostability after cyclizing any protein.<sup>8, 9</sup> This summer, Circularization of the AFP has been a wonderful addition to our exploration of this fascinating protein. It also gave us the chance to make use of the open source iGEM registry and even improve upon Heidelberg’s construct. Read about our results <a href=" | + | <p>Using Heidelberg’s intein biobrick <a href="http://parts.igem.org/Part:BBa_K1362000">BBa_K1362000</a>, we performed the intein-splicing reaction with the AFP to generate a circular protein: Icefinity. Heidelberg and other research parties have shown an increase in thermostability after cyclizing any protein.<sup>8, 9</sup> This summer, Circularization of the AFP has been a wonderful addition to our exploration of this fascinating protein. It also gave us the chance to make use of the open source iGEM registry and even improve upon Heidelberg’s construct. Read about our results <a href="https://2015.igem.org/Team:Queens_Canada/Circ_AFP">here!</a> </p> |
<p>The QGEM team worked to develop Heidelberg’s intein biobrick by adding a T7 promoter to our submitted circular AFP construct. Inserting a promoter allows our biobrick to not only be a carrier, but also be an expression construct of our circular AFP. This biobrick part <a href="http://parts.igem.org/Part:BBa_K1831000">BBa_K1831000</a>is described in more detail on our <a href="https://2015.igem.org/Team:Queens_Canada/Parts">Parts Page</a> and the iGEM registry.</p> | <p>The QGEM team worked to develop Heidelberg’s intein biobrick by adding a T7 promoter to our submitted circular AFP construct. Inserting a promoter allows our biobrick to not only be a carrier, but also be an expression construct of our circular AFP. This biobrick part <a href="http://parts.igem.org/Part:BBa_K1831000">BBa_K1831000</a>is described in more detail on our <a href="https://2015.igem.org/Team:Queens_Canada/Parts">Parts Page</a> and the iGEM registry.</p> | ||
Revision as of 14:30, 14 September 2015