Difference between revisions of "Part:BBa K3505024"

Latest revision as of 00:36, 28 October 2020

B-arrestin:TEV Protease GB compatible with B2-B5

Usage And Biology

B-arrestin has the ability to normally bind to the GPCR receptor and facilitate its endocytosis, desensitization or GPCR-independent signaling effects. The second composite of our TANGO system is a fusion of the b-arrestin-2 with the TEV protease.TEV protease recognizes and cleaves the cleavage site. This low proximity allows the TEV protease that is tagged to the βarrestin-2 carrier to cleave its substrate (TCS) .

Design Notes

The coding sequence was domesticated . We removed BsmBI ,BsaI , BtgZI, BpiI sites in order to be compatible with GoldenBraid and MoClo. The sequence is presents in pUPD2 and has overhangs compatible for Golden Braid cloning. The CDS has position B2-B5.

Figure 1.The overhangs of this part in the GoldenBraid Grammar.

Figure 2. The level 0 module : pupd2-b-arrestin-TEV protease (illustration from SnapGene)

Verification of Cloning

Fig.3:(U=Uncut C=Cut) Restriction Digestion of b-arrestin-TEV protease with SlaI, Expected bands : 2014 bp + 892 bp + 760 bp + 394 bp, Positive Result: green arrows

Sequence and Features

Assembly Compatibility:

10
INCOMPATIBLE WITH RFC[10]
Illegal SpeI site found at 1611
Illegal PstI site found at 303
Illegal PstI site found at 390
12
INCOMPATIBLE WITH RFC[12]
Illegal SpeI site found at 1611
Illegal PstI site found at 303
Illegal PstI site found at 390
21
INCOMPATIBLE WITH RFC[21]
Illegal BglII site found at 203
Illegal XhoI site found at 600
Illegal XhoI site found at 994
23
INCOMPATIBLE WITH RFC[23]
Illegal SpeI site found at 1611
Illegal PstI site found at 303
Illegal PstI site found at 390
25
INCOMPATIBLE WITH RFC[25]
Illegal SpeI site found at 1611
Illegal PstI site found at 303
Illegal PstI site found at 390
Illegal AgeI site found at 586
1000
INCOMPATIBLE WITH RFC[1000]
Illegal SapI.rc site found at 1545
Illegal SapI.rc site found at 1893

@@ Line 3: / Line 3: @@
 <partinfo>BBa_K3505024 short</partinfo>
+===Usage And Biology===
+B-arrestin has the ability to normally bind to the GPCR receptor and facilitate its endocytosis, desensitization or GPCR-independent signaling effects. The second composite of our TANGO system is a fusion of the b-arrestin-2 with the TEV protease.TEV protease recognizes and cleaves the cleavage site. This low proximity allows the TEV protease that is tagged to the βarrestin-2 carrier to cleave its substrate (TCS) .
-===Usage and Biology===
@@ Line 15: / Line 13: @@
 <p style="text-align: center;">
-     [[Image:T--Thessaly--GB-CCAT-GCTT.jpeg|900px|thumb|none|<i><b>Figure 1.</b>The overhangs of this part in the Golden Braid Grammar.</i>]]
+     [[Image:T--Thessaly--GB-CCAT-GCTT.jpeg|900px|thumb|none|<i><b>Figure 1.</b>The overhangs of this part in the GoldenBraid Grammar.</i>]]
@@ Line 21: / Line 19: @@
 ===Verification of Cloning===
-[[File:T--Thessaly--b-arrestin-digestion.png|700px|thumb|none|<i><b>Fig.1:</b>(U=Uncut C=Cut) Restriction Digestion of b-arrestin-TEV protease with SlaI, Expected bands : 2014 bp + 892 bp + 760 bp + 394 bp, Positive Result: green arrows</i>]]
+[[File:T--Thessaly--b-arrestin-digestion.png|700px|thumb|none|<i><b>Fig.3:</b>(U=Uncut C=Cut) Restriction Digestion of b-arrestin-TEV protease with SlaI, Expected bands : 2014 bp + 892 bp + 760 bp + 394 bp, Positive Result: green arrows</i>]]
 ===Sequence and Features===
 <partinfo>BBa_K3505024 SequenceAndFeatures</partinfo>