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<img class="ui medium image" src="https://static.igem.org/mediawiki/2016/d/dd/T--Slovenia--4.10.1.png"> | <img class="ui medium image" src="https://static.igem.org/mediawiki/2016/d/dd/T--Slovenia--4.10.1.png"> | ||
<figcaption><b>(A) Chemical structure of rapamycin. Binding sites for FRB and FKBP are shown. (B) Schematic presentation of FKBP and FRB binding to | <figcaption><b>(A) Chemical structure of rapamycin. Binding sites for FRB and FKBP are shown. (B) Schematic presentation of FKBP and FRB binding to | ||
− | rapamycin</b><br/ | + | rapamycin</b><br/><x-ref>Banaszynski</x-ref></figcaption> |
− | + | </figure> | |
</div> | </div> | ||
Revision as of 21:55, 15 October 2016
nbsp;Split proteases
The split protein system based on the inducible dimerization is an attractive method to regulate the protease activity. Wehr et al.
Our team hypothesized that the same inducible dimerization approach could also be used with TEVp homologues. We converted all of the tested orthogonal potyviral proteases
to split proteases by splitting them at positions corresponding to the position of the previously described split TEV protease. We selected three different types of
dimerization domains to induce the activity of the split proteases. The first pair of dimerization domains was the rapamycin responsive FKBP/FRB system
Interactions among different proteins play a key role among all living organisms. Chemically induced dimerization (CID) is one of such interactions,
which allows two different protein domains to dimerize after the addition of a small molecule. The most widely used CID to date is the FKBP/FRB system
which heterodimerizes upon rapamycin addition
Rapamycin is a 31-membered macrolide antifungal antibiotic that was first isolated from the Streptomyces hygroscopicus and binds with high affinity to the
12-kDa FK506 binding protein (FKBP) as well as to a 100-aminoacid domain (E2015 to Q2114) of the mammalian target of rapamycin (mTOR) protein known as the
FKBP-rapamycin binding domain (FRB) (4.10.1.)