Difference between revisions of "Team:ZJU-China/Design/Toxinmanufacture"

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     <p class="p1"> Tcs are composed of TcA, TcB, and TcC. TcA is supposed to perforate the membrane by forming channel outside-in and translocating the toxic enzymes into the host. Meanwhile the TcB and TcC cooperate with a syringe-like mechanism during membrane insertion(14). </p>  
 
     <p class="p1"> Tcs are composed of TcA, TcB, and TcC. TcA is supposed to perforate the membrane by forming channel outside-in and translocating the toxic enzymes into the host. Meanwhile the TcB and TcC cooperate with a syringe-like mechanism during membrane insertion(14). </p>  
 
     <p class="p1"> In a 2008 study, researchers expressed tcdA1 and tcdB1 in <i> <i> Enterobacter cloacae </i> </i> and fed the termites with <i> E. cloacae </i> to control termites(15). Inspired by their experiment, we chose to express tcdA1 (Uniprot: Q7N7Y9_PHOLL) and tcdB1(Uniprot: Q7N7Z0_PHOLL) to kill termites. For more details, please go to <a href="https://2015.igem.org/Team:ZJU-China/Parts" title="part page"> parts </a> </p>  
 
     <p class="p1"> In a 2008 study, researchers expressed tcdA1 and tcdB1 in <i> <i> Enterobacter cloacae </i> </i> and fed the termites with <i> E. cloacae </i> to control termites(15). Inspired by their experiment, we chose to express tcdA1 (Uniprot: Q7N7Y9_PHOLL) and tcdB1(Uniprot: Q7N7Z0_PHOLL) to kill termites. For more details, please go to <a href="https://2015.igem.org/Team:ZJU-China/Parts" title="part page"> parts </a> </p>  
     <h3> Plu1537: Bt HOMOLOGOUS TOXIC PROTEIN </h3>  
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<h3> Plu1537: Bt HOMOLOGOUS TOXIC PROTEIN </h3>  
 
     <p class="p1"> The exact function of Plu1537 is still unclear, but a research in 2009 indicated that Plu1537 <i> had insecticidal activity against Galleria larvae </i> (16). </p>  
 
     <p class="p1"> The exact function of Plu1537 is still unclear, but a research in 2009 indicated that Plu1537 <i> had insecticidal activity against Galleria larvae </i> (16). </p>  
 
     <p class="p1"> Judging that the Plu1537 protein has 30% predicted amino acid sequence similarity to a 13.6 kDa insecticidal crystal protein cry34Ab1(figure 12) in <i> Bacillus thuringiensis </i> (Uniprot: Q939T0_BACTU), which belongs to Bt crystal protein family, it may have similar toxic effect with cry34Ab1 Bt protein. </p>  
 
     <p class="p1"> Judging that the Plu1537 protein has 30% predicted amino acid sequence similarity to a 13.6 kDa insecticidal crystal protein cry34Ab1(figure 12) in <i> Bacillus thuringiensis </i> (Uniprot: Q939T0_BACTU), which belongs to Bt crystal protein family, it may have similar toxic effect with cry34Ab1 Bt protein. </p>  
     <p class="p1"> Bt protein may be the most well-known toxic protein till now. It is widely used in transgene plants to kill the larvae of worm. It also “interacts with membranes to form pores”(17). And there are abundant evidences to ensure the safety of Bt protein(更详细?). </p>  
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     <p class="p1"> Bt protein may be the most well-known toxic protein till now. It is widely used in transgene plants to kill the larvae of worm. It also “interacts with membranes to form pores”(17). And there is abundant evidence to ensure the safety of Bt protein. </p>  
 
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     <p class="p1"> We have successfully cloned the <i> plu1537 </i> gene and expressed the Plu1537 toxin protein in <i> E.coli </i> <i> BL21 (DE3) </i> , for more details, please go to </p>  
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     <p class="p1"> We have successfully cloned the plu1537 gene and expressed the Plu1537 toxin protein in <i> E.coli </i> <i> BL21 (DE3) </i> , for more details, please go to </p>  
 
     <h3> Plu0840: ENTEROTOXIN Ast HOMOLOGOUS PROTEIN </h3>  
 
     <h3> Plu0840: ENTEROTOXIN Ast HOMOLOGOUS PROTEIN </h3>  
 
     <p class="p1"> The exact function of Plu0840 is also unclear. A 2007 study confirmed that Plu0840 had weak oral toxicity against two kinds of moth ( <i> S. litura and S. exigua </i> )(13). </p>  
 
     <p class="p1"> The exact function of Plu0840 is also unclear. A 2007 study confirmed that Plu0840 had weak oral toxicity against two kinds of moth ( <i> S. litura and S. exigua </i> )(13). </p>  

Revision as of 15:04, 17 September 2015

Toxin Manufacture

Introduction

Biological pesticides can be divided into two types: small molecular compounds and biological macromolecules. On the one hand, small compounds are more prone to be absorbed by termites while more costly to produce. On the other hand, macromolecules are easier and cheaper to produce whereas sometimes not as effective as small molecules. Hence, to kill termites more efficiently and effectively, we choose both--We plan to overexpress avermectin in its host Streptomyces avermitilis and express four kinds of toxic protein in Escherichia coli BL21 (DE3) . Then we embed the engineered S. avermitilis and E.coli with CNC carrier and feed termites with the CNC imbedded bacteria. For more information about CNC, please go to the main page of CNC .

Avermectin manufacture

Judging that many toxic small compounds are harmful to human being, we choose avermectin, which is highly specific to insects and does little harm to human. For one thing, being a secondary metabolite produced by Streptomyces avermitilis , avermectin is encoded by an 80kb gene cluster, making it difficult to be engineered in other standardized strains, for instance, Escherichia coli . For another, the avermectin yield in wild type S. avermitilis strain is comparatively low. Nevertheless, we plan to engineer the wild S. avermitilis to improve the yield of avermectin, embed the engineered strain with CNC and feed termites with CNC embedded S. avermitilis .

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Toxic protein manufacture

In order to kill the termites, we have chosen four types of insecticidal toxic proteins, respectively Tc protein tcdA1, tcdB1, bt-like Plu0840 and enterotoxin-like Plu1537, from Photorhabdus luminescens TT01, a bacterium of native toxin storehouse. Then we clone these genes from the genome of TT01 , construct corresponding vectors, successfully express these proteins in Escherichia coli BL21 (DE3) and feed the termites with the raw engineered BL21 embedded with CNC. For more information about CNC, please go to the main page of CNC.

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Reference

1. X. Zhang et al., APPL MICROBIOL BIOT 72, 986 (2006-09-27, 2006).

2. H. Ikeda, K. Shin-ya, S. Omura, J IND MICROBIOL BIOT 41, 233 (2014).

3. H. Ikeda et al., NAT BIOTECHNOL 21, 526 (2003).

4. P. MAZODIER, R. PETTER, C. THOMPSON, J BACTERIOL 171, 3583 (1989).

5. F. Flett, V. Mersinias, C. P. Smith, FEMS MICROBIOL LETT 155, 223 (1997).

6. 孙宁, 浙江大学 (2013).

7. D. J. MACNEIL, J BACTERIOL 170, 5607 (1988).

8. R. K. Holmes, M. G. Jobling, (1996-01-19, 1996).

9. J. A. HEINEMANN, G. F. SPRAGUE, NATURE 340, 205 (1989).

10. T. Kunik et al., P NATL ACAD SCI USA 98, 1871 (2001).

11. V. L. Waters, NAT GENET 29, 375 (2001).

12. E. Duchaud et al., NAT BIOTECHNOL 21, 1307 (2003).

13. M. Li, L. H. Qiu, Y. Pang, ANN MICROBIOL 57, 313 (2007).

14. C. Gatsogiannis et al., NATURE 495, 520 (2013-03-20, 2013).

15. R. Zhao et al., APPL ENVIRON MICROB 74, 7219 (2008-12-01, 2008).

16. M. Li et al., MOL BIOL REP 36, 785 (2009).

17. M. S. Kelker et al., PLOS ONE 9, (2014).

18. J. Sha, E. V. Kozlova, A. K. Chopra, INFECT IMMUN 70, 1924 (2002).



Toxin manufacture





termit