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<p style="text-indent:2em">To test the reporter system, we cultured a mosquito Aedes albopictus C6/36 cell line and transfected cells with the plasmid of Ac5-GFP-polyA. GFP positive cells and intensity were analyzed 2 days after transfection.</p> | <p style="text-indent:2em">To test the reporter system, we cultured a mosquito Aedes albopictus C6/36 cell line and transfected cells with the plasmid of Ac5-GFP-polyA. GFP positive cells and intensity were analyzed 2 days after transfection.</p> | ||
− | <h3> | + | <h3>EXPERIMENT</h3> |
− | <p | + | <p>↓C6/36 cells (1.8 x 105 cells/well in a 96-well plate) |
+ | ↓Liposome-mediated transfection and culture for 2 more days | ||
+ | ↓Read fluorescence intensity at Ex/Em = 480/520 nm with a microplate reader | ||
+ | ↓Observe GFP+ cells under a fluorescence microscope</p> | ||
<p style="text-indent:2em">In addition, it is usually reported that more often children rather than adults die from acute aflatoxicosis because adults have higher tolerance for aflatoxin. Despite a certain extent of tolerance in adults, aflatoxins are yet to be feared since they are well-known mycotoxins for their chronic carcinogenesis. AFB1 is the most potent hepatocarcinogen in mammals and it is included in category 1A<sub>[6]</sub>. When aflatoxins are taken into the body, they will first undergo phaseⅠmetabolism in liver. There are a group of heme-binding enzymes called cytochrome P450 (CYP450) involving in the metabolism of endogenous substrates and biotransformation of xenobiotics like aflatoxins. When AFB1 is metabolized into AFB1-exo-8,9-epoxide (AFBO), it can bind to DNA and form DNA adducts<sub>[1]</sub>. If this damage cannot be repaired, it will lead to mutation and probably result in cancer.</p> | <p style="text-indent:2em">In addition, it is usually reported that more often children rather than adults die from acute aflatoxicosis because adults have higher tolerance for aflatoxin. Despite a certain extent of tolerance in adults, aflatoxins are yet to be feared since they are well-known mycotoxins for their chronic carcinogenesis. AFB1 is the most potent hepatocarcinogen in mammals and it is included in category 1A<sub>[6]</sub>. When aflatoxins are taken into the body, they will first undergo phaseⅠmetabolism in liver. There are a group of heme-binding enzymes called cytochrome P450 (CYP450) involving in the metabolism of endogenous substrates and biotransformation of xenobiotics like aflatoxins. When AFB1 is metabolized into AFB1-exo-8,9-epoxide (AFBO), it can bind to DNA and form DNA adducts<sub>[1]</sub>. If this damage cannot be repaired, it will lead to mutation and probably result in cancer.</p> | ||
<img class="pic" src="https://static.igem.org/mediawiki/2017/c/c1/T--CSMU_NCHU_Taiwan--ProjectDescription2.png" style="width:60%"> | <img class="pic" src="https://static.igem.org/mediawiki/2017/c/c1/T--CSMU_NCHU_Taiwan--ProjectDescription2.png" style="width:60%"> |
Revision as of 06:20, 18 September 2018