Difference between revisions of "Part:BBa K4040020"

Revision as of 11:40, 11 October 2021

Synthetic Receptor GP130-TEV

Sequence and Features

Assembly Compatibility:

10
COMPATIBLE WITH RFC[10]
12
COMPATIBLE WITH RFC[12]
21
INCOMPATIBLE WITH RFC[21]
Illegal BamHI site found at 1508
23
COMPATIBLE WITH RFC[23]
25
COMPATIBLE WITH RFC[25]
1000
COMPATIBLE WITH RFC[1000]

Usage and Biology

Based on the mechanism of Tango/MESA, we bind TEV-protase to GP130. We used CMV as the promoter. When the concentration of IL-6 rises to a certain level, IL-6 binds to mIL-6R (membrane-bound IL-6R), homodimerization of gp130 is induced. A high-affinity functional receptor complex of IL-6, IL-6R and gp130 is formed. Then, TEV-protase connected behind is activated. TEV-protase binds to TCS and releases transcription factors on the other two receptors through enzyme digestion to initiate the subsequent pathway.

Figure1.The structure of gp130-TEV.

@@ Line 7: / Line 7: @@
 Based on the mechanism of Tango/MESA, we bind TEV-protase to GP130. We used CMV as the promoter. When the concentration of IL-6 rises to a certain level, IL-6 binds to mIL-6R (membrane-bound IL-6R), homodimerization of gp130 is induced. A high-affinity functional receptor complex of IL-6, IL-6R and gp130 is formed.  Then, TEV-protase connected behind is activated. TEV-protase binds to TCS and releases transcription factors on the other two receptors through enzyme digestion to initiate the subsequent pathway.
-[[File:T--NMU_China--gp130-tev.jpg|300px|thumb|left|<b>Figure1.</b>Vector maps of tested CAR designs and schematics showing the structures of CARs.]]
+[[File:T--NMU_China--gp130-tev.jpg|300px|thumb|left|<b>Figure1.</b>The structure of gp130-TEV.]]
 <!-- Add more about the biology of this part here