Team:Tec-Monterrey/projectmodeling/construct2
From 2011.igem.org
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Our most promising construct was our first “Extracellular Expression Device”, mediated by an Auto-transporter membrane protein complex. For this device we characterized two new parts, and was made up of five parts. We used an arabinose induced promoter Pbad (BBa_K206000) and its repressor enzyme AraC (BBa_I13458), followed next by one of our first part BBa_K633002, made out of Ribosome binding site (BBa_b0034) and our signal peptide phoA and enzyme cellulase. Our second part BBa_K6330014, the extracellular expressing complex made out of a linker followed by our auto-transporter membrane protein estA. | Our most promising construct was our first “Extracellular Expression Device”, mediated by an Auto-transporter membrane protein complex. For this device we characterized two new parts, and was made up of five parts. We used an arabinose induced promoter Pbad (BBa_K206000) and its repressor enzyme AraC (BBa_I13458), followed next by one of our first part BBa_K633002, made out of Ribosome binding site (BBa_b0034) and our signal peptide phoA and enzyme cellulase. Our second part BBa_K6330014, the extracellular expressing complex made out of a linker followed by our auto-transporter membrane protein estA. | ||
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