Team:Heidelberg/Project/miRNA Kit
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Laura Nadine (Talk | contribs) (→Introduction) |
Laura Nadine (Talk | contribs) (→Introduction) |
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The basic set-up of our fine tuning construct, miTuner, allows on the simultaneous expression of a synthetic miRNA and a gene of interest (GOI) that is fused with a binding site for this miRNA. Our kit comes with different parts that can be combined by choice, e. g. different mammalian promoters and characterized binding sites of specific properties. By chosing a certain binding site to tag the GOI, one can adjust the level of expression of this gene. In a proof of principle approach, we show the fine tuning capability of our set up using a [https://2010.igem.org/Team:Heidelberg/Notebook/Material_Methods#Dual_Luciferase_Assay Dual Luciferase Assay]. Here, firefly luciferase acts as the GOI targeted by a synthetic miRNA, while Renilla is used to normalize measurements. | The basic set-up of our fine tuning construct, miTuner, allows on the simultaneous expression of a synthetic miRNA and a gene of interest (GOI) that is fused with a binding site for this miRNA. Our kit comes with different parts that can be combined by choice, e. g. different mammalian promoters and characterized binding sites of specific properties. By chosing a certain binding site to tag the GOI, one can adjust the level of expression of this gene. In a proof of principle approach, we show the fine tuning capability of our set up using a [https://2010.igem.org/Team:Heidelberg/Notebook/Material_Methods#Dual_Luciferase_Assay Dual Luciferase Assay]. Here, firefly luciferase acts as the GOI targeted by a synthetic miRNA, while Renilla is used to normalize measurements. | ||
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We further tested our kit using a gene that is an interesting candidate for gene therapy, human alpha-1-antitrypsin (haat) (ref, description). In this approach, we tag haat as our GOI with binding sites that we measured and characterized with our [https://2010.igem.org/Team:Heidelberg/Project/miMeasure miMeasure] construct beforehand and wanted to test in a gene therapeutic background. | We further tested our kit using a gene that is an interesting candidate for gene therapy, human alpha-1-antitrypsin (haat) (ref, description). In this approach, we tag haat as our GOI with binding sites that we measured and characterized with our [https://2010.igem.org/Team:Heidelberg/Project/miMeasure miMeasure] construct beforehand and wanted to test in a gene therapeutic background. | ||
Revision as of 19:01, 24 October 2010
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