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assembled with a BioBrick existing part of GFP to generate | assembled with a BioBrick existing part of GFP to generate | ||
the reporter vector of Ac5-GFP-polyA / pSB1C3 (K2543004).</p> | the reporter vector of Ac5-GFP-polyA / pSB1C3 (K2543004).</p> | ||
− | + | <img class="pic" src="https://static.igem.org/mediawiki/2017/6/69/T--CSMU_NCHU_Taiwan--ProjectDescription1.png" style="width:50%"> | |
− | + | <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>The harm of Aflatoxin B1</h3> | <h3>The harm of Aflatoxin B1</h3> | ||
<p style="text-indent:2em">Aflatoxin B1 (AFB1) is the most toxic and carcinogenic in mammals. Animals that consume AFB1-contaminated food can develop acute and chronic health problems. For acute aflatoxicosis in animals, AFB1 causes liver necrosis in rats<sub>[3]</sub> and hepatitis X in dogs<sub>[4]</sub>. It also causes hemorrhagic necrosis of the liver, bile duct proliferation, edema, and lethargy in human<sub>[5]</sub>.</p> | <p style="text-indent:2em">Aflatoxin B1 (AFB1) is the most toxic and carcinogenic in mammals. Animals that consume AFB1-contaminated food can develop acute and chronic health problems. For acute aflatoxicosis in animals, AFB1 causes liver necrosis in rats<sub>[3]</sub> and hepatitis X in dogs<sub>[4]</sub>. It also causes hemorrhagic necrosis of the liver, bile duct proliferation, edema, and lethargy in human<sub>[5]</sub>.</p> |
Revision as of 05:56, 18 September 2018