Team:NYMU-Taipei/results/optomagnetic-design1
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[[Image: c1_NYMU.png|frame|none|Fig. 7: The main design construct. Ori is the origin of replication of AMB-1. Pmsp1 is the promoter for AMB-1.]] | [[Image: c1_NYMU.png|frame|none|Fig. 7: The main design construct. Ori is the origin of replication of AMB-1. Pmsp1 is the promoter for AMB-1.]] | ||
- | The correlated part of construct in Fig. 7 is <font color=deeppink>pYMB essentials+[YN-13-R]+[YC-CHAMP]</font>, links to [ | + | The correlated part of construct in Fig. 7 is <font color=deeppink>pYMB essentials+[YN-13-R]+[YC-CHAMP]</font>, links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624018 BBa_K624018]. |
[[Image: c2_NYMU.png|frame|none|Fig. 8: A construct without YC on the CHAMP is our negative control in our design. It would not light up no matter there is magnetic field applied or not.]] | [[Image: c2_NYMU.png|frame|none|Fig. 8: A construct without YC on the CHAMP is our negative control in our design. It would not light up no matter there is magnetic field applied or not.]] | ||
- | The related part of construct in Fig. 8 is <font color=deeppink>pYMB essentials+[YN-13-R]</font>, links to [ | + | The related part of construct in Fig. 8 is <font color=deeppink>pYMB essentials+[YN-13-R]</font>, links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624024 BBa_K624024]. |
[[Image: c3_NYMU.png|frame|none|Fig. 9:. We design this construct with the whole YFP on the N-terminus of Mms13 and the CHAMP design to induce the BRET phenomenon. We suppose that with the CHMAP design, the construct will light up only when magnetic force is applied.]] | [[Image: c3_NYMU.png|frame|none|Fig. 9:. We design this construct with the whole YFP on the N-terminus of Mms13 and the CHAMP design to induce the BRET phenomenon. We suppose that with the CHMAP design, the construct will light up only when magnetic force is applied.]] |
Revision as of 03:40, 6 October 2011
Contents |
Constructs and Experimental Results
We now follow the steps we construct our design to examine and illustrate what we have done so far. The total parts we constructed and their detailed information will be performed and recorded in our partsregistry pages.
The Beginning
As soon as we have the AMB-1 bacteria colony, we do the AMB-1 colony PCR to get the Mms13's DNA sequences as our parts to do the following steps.
The correcterized gel electrophoresis result is shown below.(See Figure 2) The detail of part Mms13's information: [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624005 BBa_K624005].
Construct Mms13
Then, after we have the fundamental material of Mms13, we did the next step of our construct.(See Figure 3)
The characterized and checked results shown in Figure 4.
For parts mms13-rLuc, links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624007 BBa_K624007]; YN-mms13-rLuc, links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624008 BBa_K624008]; EYFP-mms13-rLuc fusion, links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624006 BBa_K624006].
Construct CHAMP Design
As for the CHAMP part, we use ligation process to get the whole sequences of CHAMP peptides. However, we still use the recombinant PCR procedure to anchor either YC or YFP in our process. Several electrophoresis results for CHAMP constructs are shown below.
Whole Construct and Experimental Results
After we have both materials of Mms13's construction and CHAMP peptides' construction, we use ligation procedure to fulfill six constructs we design in our optomagnetic-design.
The correlated part of construct in Fig. 7 is pYMB essentials+[YN-13-R]+[YC-CHAMP], links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624018 BBa_K624018].
The related part of construct in Fig. 8 is pYMB essentials+[YN-13-R], links to [http://partsregistry.org/wiki/index.php?title=Part:BBa_K624024 BBa_K624024].