Difference between revisions of "Team:Nankai/Attributions"
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<h2 id="b" style="font-family: 'Times New Roman'; font-style: normal; font-weight: 400; font-size: 40px;"><strong> Attribution</strong></h2> | <h2 id="b" style="font-family: 'Times New Roman'; font-style: normal; font-weight: 400; font-size: 40px;"><strong> Attribution</strong></h2> | ||
| − | + | <p>Main Support</p> | |
| − | + | <table width="558" height="357" border="1"> | |
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<tr> | <tr> | ||
| − | + | <td width="178">Technical Support</td> | |
| − | + | <td width="180">Data Support</td> | |
| − | < | + | <td width="178">Fund Support</td> |
| − | + | </tr> | |
| − | + | <tr> | |
| − | + | <td height="111">Since our work was done in the Prof. Chen's and Song's labs, we have got lots of instruction from many lab members</td> | |
| − | + | <td>Ours statistics of the experiment about the function of the γ-PGA and eukaryotic expression of the HGF1 were seperately provided by Prof. Qiao Mingqiang's and Prof. Wangshufang's labs.</td> | |
| − | < | + | <td>Our fund is offered by the College of Life Sciences.</td> |
| − | + | </tr> | |
| − | + | <tr> | |
| − | </ | + | <td>Part's Synthesis</td> |
| − | < | + | <td>Experience Sharing</td> |
| − | + | <td>Opportunity</td> | |
| − | + | </tr> | |
| − | + | <tr> | |
| − | + | <td height="112">All our 15 parts of which 12 are registered are totally synthesized by IDT.</td> | |
| − | + | <td>Our neighbor TJU is very experienced in igem work. So we have learned lots of details about the project.</td> | |
| − | + | <td>Sincere thanks for this precious opportunity given by the organizer of the igem. We all gained a lot.</td> | |
| − | + | </tr> | |
| − | + | </table> | |
| − | + | <p>Ackonwledgements</p> | |
| − | + | <ul> | |
| − | + | ||
| − | + | <li>The wild type of the Bacillus amyloliquefaciens is offered by Prof. Song's lab.</li> | |
| − | + | ||
| − | + | <li>Xylr and other sequences and seven promotors were also obtained from Prof. Song's lab.</li> | |
| − | + | Lab.</li> | |
| − | + | ||
| − | + | <li>Most projects were performed by the Nankai iGEM team.</li> | |
| − | + | ||
| − | + | <li>NEFU kindly invited our team to experience their newly-established platform for making wiki.</li> | |
| − | + | ||
| − | + | <li><p>1. Ashiuchi, M., Misono, H., 2002. Biochemistry and molecular genetics of poly-γ-glutamate synthesis. Appl. Biochem. Biotechnol. 59, 9–14.</p> | |
| − | + | <p>2. Kunioka, M., 1997. Biosynthesis and chemical reactions of poly(amino acid)s from microorganisms. Appl. Microbiol. Biotechnol. 47, 469–475.</p> | |
| − | + | <p>3. Shih, I.L., Van, Y.T., 2001. The production of poly(γ-glutamic acid) from microorganism and its various applications. Bioresour. Technol. 79, 207–225.</p> | |
| − | + | <p>4. Li, C., 2002. Poly(L-glutamic acid)--anticancer drug conjugates. Adv. Drug Deliver. Rev. 54, 695–713.</p> | |
| − | < | + | <p>5. Liang, H.F., Chen, C.T., Chen, S.C., Kulkarni, A.R., Chiu, Y.L., Chen, M.C., Sung, H.W., 2006. Paclitaxel-loaded poly(γ-glutamic acid)-poly(lactide) nanoparticles as a targeted drug delivery system for the treatment of liver cancer. Biomaterials. 27, 2051–2059.</p> |
| − | <p> | + | <p>6. Richard, A., Margaritis, A., 2001. Poly (glutamic acid) for biomedical applications. Crit. Rev. Biotechnol. 21, 219–232.</p> |
| − | < | + | <p>7. Park, Y.J., Liang, J., Yang, Z., Yang, V.C., 2001. Controlled release of clot-dissolving tissue-type plasmmogen activator from a poly(L-glutamic acid) semi-interpenetrating polymer network hydrogel. J. Control. Release. 74, 243–247.</p> |
| + | <p>8. Cao, M.F., Geng, W.T., Liu, L., Song, C.J., Xie, H., Guo, W.B., Jin, Y.H., Wang, S.F., 2011. Glutamic acid independent production of poly-γ-glutamic acid by Bacillus amyloliquefaciens LL3 and cloning of pgsBCA genes. Bioresour. Technol. 102, 4251–4257.</p> | ||
| + | <p>9. Geng, W.T., Cao, M.F., Song, C.J., Xie, H., Liu, L., Yang, C., Feng, J., Zhang, W., Jin, Y.H., Du, Y., Wang, S.F., 2011. Complete genome sequence of Bacillus amyloliquefaciens LL3, which exhibits glutamic acid-independent production of poly-γ-glutamic acid. J. Bacteriol. 193, 3393–3394.</p> | ||
| + | <p>10. Feng, J., Gao, W.X., Gu, Y.Y., Zhang, W., Cao, M.F., Song, C.J., Zhang, P., Sun, M., Yang, C., Wang, S.F., 2014a. Functions of poly-gamma-glutamic acid (γ-PGA) degradation genes in γ-PGA synthesis and cell morphology maintenance. Appl. Microbiol. Biotechnol. 98, 6397–6407.</p> | ||
| + | <p>11. Uy, D., Delaunay S., Germain, P., Engasser, J.M., Goergen, J.L. 2003. Instability of glutamate production by Corynebacterium glutamicum 2262 in continuous culture using the temperature-triggered process. J. Biotech. 104, 173-184.</p></li> | ||
| + | |||
| + | </ul> | ||
</body> | </body> | ||
</html> | </html> | ||
{{Nankaifoot}} | {{Nankaifoot}} | ||
Revision as of 13:27, 13 September 2015
Your place: Home > Attributions
Attribution
Main Support
| Technical Support | Data Support | Fund Support |
| Since our work was done in the Prof. Chen's and Song's labs, we have got lots of instruction from many lab members | Ours statistics of the experiment about the function of the γ-PGA and eukaryotic expression of the HGF1 were seperately provided by Prof. Qiao Mingqiang's and Prof. Wangshufang's labs. | Our fund is offered by the College of Life Sciences. |
| Part's Synthesis | Experience Sharing | Opportunity |
| All our 15 parts of which 12 are registered are totally synthesized by IDT. | Our neighbor TJU is very experienced in igem work. So we have learned lots of details about the project. | Sincere thanks for this precious opportunity given by the organizer of the igem. We all gained a lot. |
Ackonwledgements
- The wild type of the Bacillus amyloliquefaciens is offered by Prof. Song's lab.
- Xylr and other sequences and seven promotors were also obtained from Prof. Song's lab. Lab.
- Most projects were performed by the Nankai iGEM team.
- NEFU kindly invited our team to experience their newly-established platform for making wiki.
1. Ashiuchi, M., Misono, H., 2002. Biochemistry and molecular genetics of poly-γ-glutamate synthesis. Appl. Biochem. Biotechnol. 59, 9–14.
2. Kunioka, M., 1997. Biosynthesis and chemical reactions of poly(amino acid)s from microorganisms. Appl. Microbiol. Biotechnol. 47, 469–475.
3. Shih, I.L., Van, Y.T., 2001. The production of poly(γ-glutamic acid) from microorganism and its various applications. Bioresour. Technol. 79, 207–225.
4. Li, C., 2002. Poly(L-glutamic acid)--anticancer drug conjugates. Adv. Drug Deliver. Rev. 54, 695–713.
5. Liang, H.F., Chen, C.T., Chen, S.C., Kulkarni, A.R., Chiu, Y.L., Chen, M.C., Sung, H.W., 2006. Paclitaxel-loaded poly(γ-glutamic acid)-poly(lactide) nanoparticles as a targeted drug delivery system for the treatment of liver cancer. Biomaterials. 27, 2051–2059.
6. Richard, A., Margaritis, A., 2001. Poly (glutamic acid) for biomedical applications. Crit. Rev. Biotechnol. 21, 219–232.
7. Park, Y.J., Liang, J., Yang, Z., Yang, V.C., 2001. Controlled release of clot-dissolving tissue-type plasmmogen activator from a poly(L-glutamic acid) semi-interpenetrating polymer network hydrogel. J. Control. Release. 74, 243–247.
8. Cao, M.F., Geng, W.T., Liu, L., Song, C.J., Xie, H., Guo, W.B., Jin, Y.H., Wang, S.F., 2011. Glutamic acid independent production of poly-γ-glutamic acid by Bacillus amyloliquefaciens LL3 and cloning of pgsBCA genes. Bioresour. Technol. 102, 4251–4257.
9. Geng, W.T., Cao, M.F., Song, C.J., Xie, H., Liu, L., Yang, C., Feng, J., Zhang, W., Jin, Y.H., Du, Y., Wang, S.F., 2011. Complete genome sequence of Bacillus amyloliquefaciens LL3, which exhibits glutamic acid-independent production of poly-γ-glutamic acid. J. Bacteriol. 193, 3393–3394.
10. Feng, J., Gao, W.X., Gu, Y.Y., Zhang, W., Cao, M.F., Song, C.J., Zhang, P., Sun, M., Yang, C., Wang, S.F., 2014a. Functions of poly-gamma-glutamic acid (γ-PGA) degradation genes in γ-PGA synthesis and cell morphology maintenance. Appl. Microbiol. Biotechnol. 98, 6397–6407.
11. Uy, D., Delaunay S., Germain, P., Engasser, J.M., Goergen, J.L. 2003. Instability of glutamate production by Corynebacterium glutamicum 2262 in continuous culture using the temperature-triggered process. J. Biotech. 104, 173-184.