Difference between revisions of "Part:BBa K1150021"
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− | <div align="justify"; margin-right:10px>Krüppel-associated Box repressor domains - commonly termed as | + | <div align="justify"; margin-right:10px>Krüppel-associated Box repressor domains - commonly termed as KRAB - are highly conserved polypeptide motifs and were first functionally characterized in 1991 (<i>Rosati et al.</i>, 1991). As they constitute about one third of all human zinc finger transcription factors, key regulatory features in higher eukaryotic transcriptomics are suggested (<i>Witzgall et al.</i>, 1994). Even in terms of tetrapod evolution, the role of their great abundance has been extensively discussed (<i>Birtle</i>, 2006). Even though KRAB minimal domains are usually no longer than 50-75 amino acids, their mechanism of function remains complex. </div><br> |
[[File:Freiburg2013 Plasmid Cas9-KRAB-1.jpg|800px|thumb|left|<b>Fig. 1</b> Schematic overview of dCas9-KRAB composite part with all features.]] | [[File:Freiburg2013 Plasmid Cas9-KRAB-1.jpg|800px|thumb|left|<b>Fig. 1</b> Schematic overview of dCas9-KRAB composite part with all features.]] |
Revision as of 18:31, 4 October 2013
uniCAS Repressor (SV40 promoter)
SV40:HA-NLS-dCas9-Linker-KRAB-NLS:BGH | |
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Function | Transcriptional Repression |
Use in | Mammalian cells |
RFC standard | RFC 25 |
Backbone | pSB1C3 |
Organism | Streptococcus pyogenes, Homo sapiens |
Source | Feng Zhang, Addgene Konrad Müller, University of Freiburg |
Submitted by | [http://2013.igem.org/Team:Freiburg Freiburg 2013] |
Krüppel-associated Box repressor domains - commonly termed as KRAB - are highly conserved polypeptide motifs and were first functionally characterized in 1991 (Rosati et al., 1991). As they constitute about one third of all human zinc finger transcription factors, key regulatory features in higher eukaryotic transcriptomics are suggested (Witzgall et al., 1994). Even in terms of tetrapod evolution, the role of their great abundance has been extensively discussed (Birtle, 2006). Even though KRAB minimal domains are usually no longer than 50-75 amino acids, their mechanism of function remains complex.
Usage and Biology
Sequence and Features
Assembly Compatibility:
- 10COMPATIBLE WITH RFC[10]
- 12COMPATIBLE WITH RFC[12]
- 21INCOMPATIBLE WITH RFC[21]Illegal BglII site found at 664
- 23COMPATIBLE WITH RFC[23]
- 25COMPATIBLE WITH RFC[25]
- 1000INCOMPATIBLE WITH RFC[1000]Illegal BsaI.rc site found at 4784
Illegal SapI.rc site found at 4748