Part:BBa_K3924038
GM-CSF
Sequence and Features
- 10INCOMPATIBLE WITH RFC[10]Illegal PstI site found at 7
Illegal PstI site found at 196
Illegal PstI site found at 214 - 12INCOMPATIBLE WITH RFC[12]Illegal PstI site found at 7
Illegal PstI site found at 196
Illegal PstI site found at 214 - 21COMPATIBLE WITH RFC[21]
- 23INCOMPATIBLE WITH RFC[23]Illegal PstI site found at 7
Illegal PstI site found at 196
Illegal PstI site found at 214 - 25INCOMPATIBLE WITH RFC[25]Illegal PstI site found at 7
Illegal PstI site found at 196
Illegal PstI site found at 214 - 1000INCOMPATIBLE WITH RFC[1000]Illegal BsaI site found at 62
Profile
Name: GM-CSF
Base Pairs: 435bp
Origin: Homo sapiens
Properties: A kind of colony stimulating factor.
Usage and Biology
In order to heal the intestinal tract damage, one of notable symptoms of IBD, we adopted a special therapy expressing the therapeutic proteins controllably by E.coli Nissle 1917 (EcN) in situ. The design is based on a ternary system: sensor - secretion peptide - therapeutic proteins.
GM-CSF is one of the candidate therapeutic proteins we screened out to treat IBD, which is the effector element in the ternary. It can augment the intestinal innate immune defense rather than suppressing a secondary inflammatory response and possibly to improve T regulatory cell activity which may be effective in CD.
Design and Construction
According to literature research we chose 10 candidate proteins for IBD treatment.
Table 1. List of candidate therapeutic proteins
Part Name | Element Name | Reference |
---|---|---|
BBa_K3924000 BBa_K3924001 BBa_K3924002 |
TFF1/2/3 | [1][2] |
BBa_K3924003 | Chromofungin(CHR) | [3] |
BBa_K3924004 | IL10 | [4] |
BBa_K3924005 | Defensin-5(HD5) | [5] |
BBa_K3924006 | GLP2 | [6] |
BBa_K3924007 | Fgl2 | [7] |
BBa_K3924008 | SOCS1-KIR | [3] |
BBa_K3924009 | tkip | [3] |
BBa_K3924037 | G-CSF | [8][9] |
BBa_K3924038 | GM-CSF | [8][10] |
BBa_K3924039 | Beta-defensin 4A(hBD2) | [11] |
The sequence of GM-CSF is acquired from Gene database (Gene ID: 1437).
Functional Verification
All of these proteins are worth studying, but we only chose a few proteins as a proof of concept in our actual wet lab experiments because of the time limit and the high expense of gene synthesis.
For all candidate therapeutic proteins we did codon analysis with our own software tool.(Fig 3)
As for GM-CSF, the result of codon preference is shown in Fig 4.
Reference
[1] Aamann, L., Vestergaard, E. M., & Grønbæk, H. (2014). Trefoil factors in inflammatory bowel disease. World journal of gastroenterology, 20(12), 3223–3230.
[2] Praveschotinunt, P., Duraj-Thatte, A.M., Gelfat, I. et al. Engineered E. coli Nissle 1917 for the delivery of matrix-tethered therapeutic domains to the gut. Nat Commun 10, 5580 (2019).
[3] La Manna, S., Di Natale, C., Florio, D., & Marasco, D. (2018). Peptides as Therapeutic Agents for Inflammatory-Related Diseases. International journal of molecular sciences, 19(9), 2714.
[4] Li, M. C., & He, S. H. (2004). IL-10 and its related cytokines for treatment of inflammatory bowel disease. World journal of gastroenterology, 10(5), 620–625.
[5] Shukla, P.K., Meena, A.S., Rao, V. et al. Human Defensin-5 Blocks Ethanol and Colitis-Induced Dysbiosis, Tight Junction Disruption and Inflammation in Mouse Intestine. Sci Rep 8, 16241 (2018).
[6] Duan, L., Rao, X., Braunstein, Z., Toomey, A. C., & Zhong, J. (2017). Role of Incretin Axis in Inflammatory Bowel Disease. Frontiers in immunology, 8, 1734.
[7] Zhu, Y. , Jie, Z. , Yi, F. , Chen, L. , Zhang, L. , & Fei, Y. , et al. (2018). Control of intestinal inflammation, colitis-associated tumorigenesis, and macrophage polarization by fibrinogen-like protein 2. Frontiers in Immunology, 9, 87-.
[8] Guidi, L., Mocci, G., Marzo, M., & Rutella, S. (2008). Treatment of Crohn's disease with colony-stimulating factors: An overview. Therapeutics and clinical risk management, 4(5), 927–934.
[9] Vanz, A. L. , Renard, G. , Palma, M. S. , Chies, J. M. , Dalmora, S. L. , & Basso, L. A. , et al. (2008). Human granulocyte colony stimulating factor (hg-csf): cloning, overexpression, purification and characterization. Microbial Cell Factories, 7(1), 1-12.
[10] Malekian, R., Jahanian-Najafabadi, A., Moazen, F., Ghavimi, R., Mohammadi, E., & Akbari, V. (2019). High-yield Production of Granulocyte-macrophage Colony-stimulating Factor in E. coli BL21 (DE3) By an Auto-induction Strategy. Iranian journal of pharmaceutical research : IJPR, 18(1), 469–478.
[11] Koeninger, L. , Armbruster, N. S. , Brinch, K. S. , Kjaerulf, S. , & Wehkamp, J. . (2020). Human β-defensin 2 mediated immune modulation as treatment for experimental colitis. Frontiers in Immunology, 11, 93.
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