Difference between revisions of "Team:Newcastle/Results"

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<b>4)Adaptors: </b> If the molecule is hard to detect, adaptor components can be placed before the detector unit, to convert the target molecules to something able to be sensed by the detector component. For example, for target that degrades into an easily detectable molecule, a biochemical conversion adaptor could be placed before the detector component which enzymatically degrades the target molecule into the molecule detected by the detector module.
 
<b>4)Adaptors: </b> If the molecule is hard to detect, adaptor components can be placed before the detector unit, to convert the target molecules to something able to be sensed by the detector component. For example, for target that degrades into an easily detectable molecule, a biochemical conversion adaptor could be placed before the detector component which enzymatically degrades the target molecule into the molecule detected by the detector module.
 
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<img class="mySlides" src="https://static.igem.org/mediawiki/2017/f/f6/T--Newcastle--BB_Design-0.png" width="100%">
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<img src="https://static.igem.org/mediawiki/2017/5/5e/Graphy%281%29.jpeg" class="img-fluid rounded mx-auto d-block" style="max-width: 60%" alt="">
 
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<b>Figure 3:</b> Frequency of projects based on biosensors development in iGEM. </p>
 
<b>Figure 3:</b> Frequency of projects based on biosensors development in iGEM. </p>

Revision as of 18:38, 31 October 2017

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Our Experimental Results



Below is a diagram of our Sensynova Framework. Clicking on each part of the framework (e.g. detector modules) links to the relevant results.

Alternatively, at the bottom of this page are tabs which will show you results for every part of the project



Framework

Framework Chassis

Biochemical Adaptor

Target

Detector Modules

Multicellular Framework Testing

C12 HSL: Connector 1

Processor Modules

Framework in Cell Free Protein Synthesis Systems

C4 HSL: Connector 2

Reporter Modules



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