Difference between revisions of "Team:UCL/Safety"
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We plan to characterize the level of B12-induced <i>in vivo</i> repression of downstream toxin gene by evaluating the survival of bacteria engineered with our constructs at different levels of B12 supplementation. By integrating modelling, we hope to be able to <b>fine-tune the affinity</b> of our engineered riboswitches to the level that would allow for responsivity to human gut conditions. <br><Br> | We plan to characterize the level of B12-induced <i>in vivo</i> repression of downstream toxin gene by evaluating the survival of bacteria engineered with our constructs at different levels of B12 supplementation. By integrating modelling, we hope to be able to <b>fine-tune the affinity</b> of our engineered riboswitches to the level that would allow for responsivity to human gut conditions. <br><Br> | ||
− | <img src="https://static.igem.org/mediawiki/2015/3/35/UCL_Screenshot_2015-09-01_at_13.42.40.png" style="margin: auto;"><br><br> | + | <img src="https://static.igem.org/mediawiki/2015/3/35/UCL_Screenshot_2015-09-01_at_13.42.40.png" style="margin: auto;text-align:center;"><br><br> |
</h4> | </h4> |
Revision as of 20:37, 18 September 2015
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B12 riboswitch
In order to address safety issues associated with our psychobiotics, we have developed a unique B12 riboswitch-mediated
containment strategy
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