Team:Heidelberg/Project Highlights
From 2009.igem.org
Project HighlightsWe are able to predict functional mammalian promoter sequencesWe created HEARTBEAT, a model portfolio based upon genome-wide bioinformatic analysis and fuzzy logic. We used these tools to predict promoter sequences. Then, we synthesized such sequences. We found that promoters most closely matching the model predictions work, whereas others don't. Read more about these results on the "HEARTBEAT database" page. We also present a GUI which enables you to design the promoter of your needs. We have created a functional biochemical synthesis method for the generation of promoters librariesWe developed RA-PCR, a biochemical method for the generation of randomized promoter libraries. We created a library of constitutive promoters, a NF-κB responsive promoter which underwent extensive characterization and some other regulated promoters. We have developed novel standards for measurement of promoters in mammalian cellsApplying both qRT-PCR and flow cytometry, we developed two new relative units in analogy to bacterial RPU for use in mammalians: Relative Expression Units and Relative Mammalian Promoter Units. We apply these units to the characterization of our promoters, as well as an existing [http://partsregistry.org/Part:BBa_I712004 promoter from the registry]. 4 RFCs, well characterized partsWe stick with the standards required by synthetic biology and submit all the methods and units we developed as RFCs (Request for Comments). By introducing new standards for synthetic biology in mammalian cells, we hope to set a process in motion that will skyrocket the number of mammalian parts in the registry within the next years:
We also submit more than 10 well-characterized parts to the registry (see Parts Characterization). Also, we submit several other parts, for which we ofdfer at least a rough characterization (Find our full parts list here)
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