Difference between revisions of "Team:Paris Bettencourt/Project/VitaminA"
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They were able to show that the addition of those genes to <i>Saccharomyces cerevisiae</i> was enough to make it produce beta-carotene.<br> | They were able to show that the addition of those genes to <i>Saccharomyces cerevisiae</i> was enough to make it produce beta-carotene.<br> | ||
<br><div align="center"><img src="https://static.igem.org/mediawiki/2015/9/95/ParisBettencourt_polycistron_schema.jpg" width="500px"></img></div> | <br><div align="center"><img src="https://static.igem.org/mediawiki/2015/9/95/ParisBettencourt_polycistron_schema.jpg" width="500px"></img></div> | ||
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− | < | + | <div class="column-right" align="left"><b>2A sequences or cis-acting hydrolase element:</b> <br> |
2A like sequences are able to force the ribosome to "skip" a codon. The ribosome releases the part that it has already translated and to keep translating the mRNA. It allows transcription of multiple proteins from only 1 mRNA with 1 promoter, like bacterial polycistronic elements, but also with only one kozac sequence (yeast RBS) which ensures that the quantities of all the translated product are the same.<br> | 2A like sequences are able to force the ribosome to "skip" a codon. The ribosome releases the part that it has already translated and to keep translating the mRNA. It allows transcription of multiple proteins from only 1 mRNA with 1 promoter, like bacterial polycistronic elements, but also with only one kozac sequence (yeast RBS) which ensures that the quantities of all the translated product are the same.<br> | ||
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Revision as of 19:52, 18 September 2015