Difference between revisions of "Part:BBa K2549019"
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===Biology=== | ===Biology=== | ||
+ | =====Our characterization===== | ||
+ | [[File:bestNotch.jpg|none|400px|thumb|'''Flow cytometry results of SynNotch activation.''' surAg, surface antigens, which was surface-expressed CD19 for αCD19-SynNotch or surface-expressed EGFP for LaG-SynNotch, respectively. Without surAg, the EGFP (Y axis, driven by tTAA released after SynNotch activation) was low, and it went high after adding surAg. More details please visit http://2018.igem.org/Team:Fudan/Results and http://2018.igem.org/Team:Fudan/Optimization .]] | ||
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+ | It is obvious that LaG16-2-mN1c-tTAA can be significantly activated by surface-expressed EGFP. | ||
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=====SynNotch receptors function well in Morsut L et al 2016===== | =====SynNotch receptors function well in Morsut L et al 2016===== | ||
Revision as of 17:18, 17 October 2018
LaG16-2-mN1c-tTAA
This part is the second version of our SynNotch receptors, as original published[1]. LaG16-2 (Part:BBa_K2446058) is used as the extracellular sensor module to receive the signal input from GFP. mN1c (Part:BBa_K2549006) is served as the transmembrane core domain of SynNotch, which is evident to have a low basal expression and a high activation efficiency. tTAA (Part:BBa_K2446057) is an improved tetracycline-controlled transactivator[2], which is cleaved after SynNotch activation and drives the expression of the amplifier.
Sequence and Features
- 10COMPATIBLE WITH RFC[10]
- 12COMPATIBLE WITH RFC[12]
- 21INCOMPATIBLE WITH RFC[21]Illegal BglII site found at 381
- 23COMPATIBLE WITH RFC[23]
- 25INCOMPATIBLE WITH RFC[25]Illegal NgoMIV site found at 2580
- 1000INCOMPATIBLE WITH RFC[1000]Illegal SapI.rc site found at 1495
Biology
Our characterization
It is obvious that LaG16-2-mN1c-tTAA can be significantly activated by surface-expressed EGFP.
SynNotch receptors function well in Morsut L et al 2016
Please refer to the original article for more details.
Characterization
It works as we designed.
It is obvious that LaG16-2-mN1c-tTAA can be significantly activated by surface-expressed EGFP.
References
- ↑ Engineering Customized Cell Sensing and Response Behaviors Using Synthetic Notch Receptors. Morsut L, Roybal KT, Xiong X, ..., Thomson M, Lim WA. Cell, 2016 Feb;164(4):780-91 PMID: 26830878; DOI: 10.1016/j.cell.2016.01.012
- ↑ Exploring the sequence space for tetracycline-dependent transcriptional activators: novel mutations yield expanded range and sensitivity. Urlinger S, Baron U, Thellmann M, ..., Bujard H, Hillen W. Proc Natl Acad Sci U S A, 2000 Jul;97(14):7963-8 PMID: 10859354