Difference between revisions of "Team:Nottingham/Achievements"

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The asRNA parts were created to target the two well characterised <em>C. difficile</em> toxins, TcdA and TcdB. These toxins are responsible for the characteristic symptoms of <em>C. difficile</em> infection. The parts were constructed in such a way that they targeted both toxins simultaneously because both toxins have been shown to have independent roles.<p>
 
The asRNA parts were created to target the two well characterised <em>C. difficile</em> toxins, TcdA and TcdB. These toxins are responsible for the characteristic symptoms of <em>C. difficile</em> infection. The parts were constructed in such a way that they targeted both toxins simultaneously because both toxins have been shown to have independent roles.<p>
  
<img style="width:100%" src="https://static.igem.org/mediawiki/2018/e/ed/T--Nottingham--asRNA_construct_one_1.png"><img style="width:100%" src="https://static.igem.org/mediawiki/2018/1/15/T--Nottingham--asRNA_construct_two_1.png">
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<img style="width:100%" src="https://static.igem.org/mediawiki/2018/a/a9/T--Nottingham--asRNA_construct_one_2.png"><img style="width:100%" src="https://static.igem.org/mediawiki/2018/7/7c/T--Nottingham--asRNA_construct_two_2.png">
  
 
<p>The asRNA parts are downstream of a PCac_thl promoter and a PCsp_fdx promoter. Between, the promoter-asRNA pairs, there is a transcriptional terminator (fdx). As a result of GusA and GFP assays, we determined that PCac_thl promoter was the strongest promoter, followed by PCsp_fdx promoter in <em>C. difficile</em>. Together, the basic parts produced our composite part.<p>
 
<p>The asRNA parts are downstream of a PCac_thl promoter and a PCsp_fdx promoter. Between, the promoter-asRNA pairs, there is a transcriptional terminator (fdx). As a result of GusA and GFP assays, we determined that PCac_thl promoter was the strongest promoter, followed by PCsp_fdx promoter in <em>C. difficile</em>. Together, the basic parts produced our composite part.<p>
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<strong>Cytotoxicity of <em>C. difficile</em> supernatants.</strong>The graph shows supernatant cytotoxicity over a period of 120 hours. There is considerably less toxin production by <em>C. difficile</em> containing asRNA construct 1 and <em>C. difficile</em> containing asRNA construct 2 than by wild type <em>C. difficile</em>.</h6>
 
<strong>Cytotoxicity of <em>C. difficile</em> supernatants.</strong>The graph shows supernatant cytotoxicity over a period of 120 hours. There is considerably less toxin production by <em>C. difficile</em> containing asRNA construct 1 and <em>C. difficile</em> containing asRNA construct 2 than by wild type <em>C. difficile</em>.</h6>
 
          
 
          

Revision as of 19:56, 17 October 2018

Clostridium dTox Project Human Practices Public Engagement Lab Modelling Collaborations Achievements Team Attributions