pBT3-N膜蛋白酵母双杂交系统载体-BioVector NTCC质粒载体菌种细胞蛋白抗体基因保藏中心
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- 货 号:pBT3-N膜蛋白酵母双杂交系统载体
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质粒类型: | 膜蛋白酵母双杂交系统 |
---|---|
启动子: | CYC1 |
载体大小: | 7608 bp |
筛选标记: | LEU2 |
载体抗性: | Kanamycin |
质粒图谱
Position Feature Position Feature
Start: 62 End: 352 CYC1 promoter Start: 2499 End: 4709 LEU2 auxotrophic marker
Start: 364 End: 969 LexA DNA binding domain Start: 4858 End: 5891 KanR resistance gene
Start: 988 End: 1224 VP16 transactivation domain Start: 6184 End: 6851 pBluescript origin of replication
Start: 1231 End: 1365 Cub, amino acids 34-76 of ubiquitin Start: 6973 End: 7512 CEN/ARS origin of replication
Start: 1509 End: 1768 CYC1 terminator
Multispan integral membrane proteins (i.e. those having multiple transmembrane domains)
with an Nout/Cin topology often do not have a signal sequence. We recommend that you use
the vector pBT3-STE for these proteins. The STE2 leader sequence in pBT3-STE is derived
from the Saccharomyces cerevisiae Ste2 protein (a G protein coupled receptor). It does not
have any targeting function but only serves as a short leader sequence to optimize expression
of your bait. The Cub-LexA-VP16 cassette is fused to the C-terminus of the bait.
On the other hand, if you have a protein whose C-terminus is lumenal, you should use
pBT3-N to fuse the LexA-VP16-Cub module to the cytosolic N-terminus of your protein of
interest. The vector pBT3-N is specifically designed for screening type II integral membrane
proteins.
Subclone the cDNA encoding your type II
protein into the vector pBT3-N. No leader
sequence is required. Please note that the
orientation of the module is reversed in
pBT3-N (LexA-VP16-Cub) to allow
separation of the transcription factor from
the bait via UBP cleavage.
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