Team:Warwick/Parts/IRES
From 2014.igem.org
(Difference between revisions)
Line 104: | Line 104: | ||
IRES was shown to be 30-fold more | IRES was shown to be 30-fold more | ||
- | efficient however had never been previously used in Huh7.</p> | + | efficient however had never been previously used in Huh7.</p> <br><br> |
<h2> Click <a href="http://parts.igem.org/wiki/index.php?title=Part:BBa_K1442023">here</a> to learn about our EMCV IRES. </h2> | <h2> Click <a href="http://parts.igem.org/wiki/index.php?title=Part:BBa_K1442023">here</a> to learn about our EMCV IRES. </h2> |
Revision as of 23:34, 16 October 2014
IRES
This acts as an initiation for eukaryotic ribosomes and begins translation of the following protein sequence. We compared two different IRESs: the classical EMCV IRES used in many papers,which has been shown to be compatible with replicons and the NKRF IRES derived from the 3’UTR of the mammalian NF-kappaB repressing factor, which we also chose to test because during investigation regarding the efficacy and strength of the EMCV IRES, the NKRF derived IRES was shown to be 30-fold more efficient however had never been previously used in Huh7.