Difference between revisions of "Team:CGU Taiwan/Entrepreneurship"

Line 407: Line 407:
  
 
<b><font size="6px">Marketing</font></b>
 
<b><font size="6px">Marketing</font></b>
<div style="color:black;text-decoration:none;font-size:18px;margin-left:70px;">
+
<div style="color:black;text-decoration:none;font-size:18px;margin-right:10%;">
 
The number of vaccination per person is increasing while the number of vaccine-preventable diseases is also increasing. This situation accelerates virus recombination and evolution, thus, new approach is necessary for vaccine industry. Furthermore, therapeutic vaccines that target specific antigens develop rapidly in oncology and immune diseases, heralding a new vaccine market.<br>
 
The number of vaccination per person is increasing while the number of vaccine-preventable diseases is also increasing. This situation accelerates virus recombination and evolution, thus, new approach is necessary for vaccine industry. Furthermore, therapeutic vaccines that target specific antigens develop rapidly in oncology and immune diseases, heralding a new vaccine market.<br>
 
In our own survey, we made a questionnaire for public to figure out the demands of indirectly customers. For integrated marketing, we also interviewed with several experts of both basic research, industries and the hospital system (<a href="https://2016.igem.org/Team:CGU_Taiwan/Human_Practices_Survey#anchor3">read more</a>). In the future, we will collect information from our main customers in a large scale and further analyze the data to solid our business model.<br>
 
In our own survey, we made a questionnaire for public to figure out the demands of indirectly customers. For integrated marketing, we also interviewed with several experts of both basic research, industries and the hospital system (<a href="https://2016.igem.org/Team:CGU_Taiwan/Human_Practices_Survey#anchor3">read more</a>). In the future, we will collect information from our main customers in a large scale and further analyze the data to solid our business model.<br>
Line 414: Line 414:
  
 
<b><font size="6px">Law and regulation </font></b>
 
<b><font size="6px">Law and regulation </font></b>
<div style="color:black;text-decoration:none;font-size:18px;margin-left:70px;">
+
<div style="color:black;text-decoration:none;font-size:18px;margin-right:10%;">
 
FDA is the main administrative organ managing pharmaceutical products in Taiwan, following the acts of GMP and ISO. The environmental impact, safety, and production issues are also under our concern. Detail information is written in our integrated HP wiki page.</div>
 
FDA is the main administrative organ managing pharmaceutical products in Taiwan, following the acts of GMP and ISO. The environmental impact, safety, and production issues are also under our concern. Detail information is written in our integrated HP wiki page.</div>
 
<br><br>
 
<br><br>
  
 
<b><font size="6px">Progress</font></b>  
 
<b><font size="6px">Progress</font></b>  
<div style="color:black;text-decoration:none;font-size:18px;margin-left:70px;"><br>
+
<div style="color:black;text-decoration:none;font-size:18px;margin-right:10%;"><br>
 
<img src="https://static.igem.org/mediawiki/2016/4/4d/EN2.jpeg" width=850px height=400px></img><br><br>
 
<img src="https://static.igem.org/mediawiki/2016/4/4d/EN2.jpeg" width=850px height=400px></img><br><br>
 
We have proven that Leishmania could activate CD4 T cell pathway inducing efficient humoral immune response. In Further study, we will change the well-established OVA protein into our target protein from hepatitis C virus, plasmodium and tuberculosis. Since Leishmania can also be used as treatment drugs toward cytotoxic pathway, it is possible that generate both therapeutic and prophylactic drugs toward Leishmania system. Leijuvant targets diseases that are under rare medical conditions which correspond to the applicant qualifications of orphan drug. In order to benefit patients suffering from diseases without efficient drugs, FDA fastens the process of orphan drug development clinical trial phase 3, accelerating the procedure of leijuvant launched on the market and reducing the cost. The orphan drug application will be summited after preclinical trial is completed. Patent application will also be submitted before clinical trial start. In our blue plan, we will finish preclinical trial and clinical trial in 7 and 4 years respectively and launch leijuvant in 2029.
 
We have proven that Leishmania could activate CD4 T cell pathway inducing efficient humoral immune response. In Further study, we will change the well-established OVA protein into our target protein from hepatitis C virus, plasmodium and tuberculosis. Since Leishmania can also be used as treatment drugs toward cytotoxic pathway, it is possible that generate both therapeutic and prophylactic drugs toward Leishmania system. Leijuvant targets diseases that are under rare medical conditions which correspond to the applicant qualifications of orphan drug. In order to benefit patients suffering from diseases without efficient drugs, FDA fastens the process of orphan drug development clinical trial phase 3, accelerating the procedure of leijuvant launched on the market and reducing the cost. The orphan drug application will be summited after preclinical trial is completed. Patent application will also be submitted before clinical trial start. In our blue plan, we will finish preclinical trial and clinical trial in 7 and 4 years respectively and launch leijuvant in 2029.
Line 427: Line 427:
  
 
<b><font size="6px">Leijuvant production (mimic real-world conditions)</font></b>
 
<b><font size="6px">Leijuvant production (mimic real-world conditions)</font></b>
<div style="color:black;text-decoration:none;font-size:18px;margin-left:70px;"><br>
+
<div style="color:black;text-decoration:none;font-size:18px;margin-right:10%;"><br>
 
<img src="https://static.igem.org/mediawiki/2016/0/0a/Leijuvant_%E6%B5%81%E7%A8%8B%E5%9C%96.png" width=850px height=150px></img><br><br>
 
<img src="https://static.igem.org/mediawiki/2016/0/0a/Leijuvant_%E6%B5%81%E7%A8%8B%E5%9C%96.png" width=850px height=150px></img><br><br>
 
Suppose our target antigen is an unknown virus. First, enter the antigen sequence into the MHC peptide prediction system, McHug, to analysis the MHC binding affinity and other basic features. And get the antigen sequence of your interest. Construct the sequence into shuttle vector to maximize the production of the antigen. Transfect the vectors into Leishmania through electroporation. Through drug selection we can select the successfully transfected Leishmania and mass culture it. Then we will use double-photo inactivation system to completely remove its infectiousness. Repeat the same process and we can design and produce different antigen specific leijuvant.<br>
 
Suppose our target antigen is an unknown virus. First, enter the antigen sequence into the MHC peptide prediction system, McHug, to analysis the MHC binding affinity and other basic features. And get the antigen sequence of your interest. Construct the sequence into shuttle vector to maximize the production of the antigen. Transfect the vectors into Leishmania through electroporation. Through drug selection we can select the successfully transfected Leishmania and mass culture it. Then we will use double-photo inactivation system to completely remove its infectiousness. Repeat the same process and we can design and produce different antigen specific leijuvant.<br>
Line 434: Line 434:
  
 
<b><font size="6px">Sponsor</font></b>
 
<b><font size="6px">Sponsor</font></b>
<div style="color:black;text-decoration:none;font-size:18px;margin-left:70px;">
+
<div style="color:black;text-decoration:none;font-size:18px;margin-right:10%;">
 
We will solicit cooperation with pharmaceutical companies that produce vaccines and adjuvants, such as GSK, Merck, Novartis, Pfizer and Sanofi. Project could be improved and process more smoothly toward discussion that combine both scientific and business perception.  
 
We will solicit cooperation with pharmaceutical companies that produce vaccines and adjuvants, such as GSK, Merck, Novartis, Pfizer and Sanofi. Project could be improved and process more smoothly toward discussion that combine both scientific and business perception.  
 
</div>
 
</div>

Revision as of 14:36, 1 December 2016


Entrepreneurship


Motivation and Goal
One reason that some severe diseases do not have efficient vaccine is the lack of T cell pathway activation. Due to this finding, leijuvant purpose to directly activate CD4 T cell pathway, and further induced better antibody production. Leijuvant prevent people from infectious diseases that do not have proper drugs, including tuberculosis, malaria and hepatitis C. With leijuvant, hundreds and thousands of people will be saved. Leijuvant has several advantages as a vaccine adjuvant, providing us with a new perspective of protecting ourselves.


Business model


Marketing
The number of vaccination per person is increasing while the number of vaccine-preventable diseases is also increasing. This situation accelerates virus recombination and evolution, thus, new approach is necessary for vaccine industry. Furthermore, therapeutic vaccines that target specific antigens develop rapidly in oncology and immune diseases, heralding a new vaccine market.
In our own survey, we made a questionnaire for public to figure out the demands of indirectly customers. For integrated marketing, we also interviewed with several experts of both basic research, industries and the hospital system (read more). In the future, we will collect information from our main customers in a large scale and further analyze the data to solid our business model.


Law and regulation
FDA is the main administrative organ managing pharmaceutical products in Taiwan, following the acts of GMP and ISO. The environmental impact, safety, and production issues are also under our concern. Detail information is written in our integrated HP wiki page.


Progress



We have proven that Leishmania could activate CD4 T cell pathway inducing efficient humoral immune response. In Further study, we will change the well-established OVA protein into our target protein from hepatitis C virus, plasmodium and tuberculosis. Since Leishmania can also be used as treatment drugs toward cytotoxic pathway, it is possible that generate both therapeutic and prophylactic drugs toward Leishmania system. Leijuvant targets diseases that are under rare medical conditions which correspond to the applicant qualifications of orphan drug. In order to benefit patients suffering from diseases without efficient drugs, FDA fastens the process of orphan drug development clinical trial phase 3, accelerating the procedure of leijuvant launched on the market and reducing the cost. The orphan drug application will be summited after preclinical trial is completed. Patent application will also be submitted before clinical trial start. In our blue plan, we will finish preclinical trial and clinical trial in 7 and 4 years respectively and launch leijuvant in 2029.


Leijuvant production (mimic real-world conditions)



Suppose our target antigen is an unknown virus. First, enter the antigen sequence into the MHC peptide prediction system, McHug, to analysis the MHC binding affinity and other basic features. And get the antigen sequence of your interest. Construct the sequence into shuttle vector to maximize the production of the antigen. Transfect the vectors into Leishmania through electroporation. Through drug selection we can select the successfully transfected Leishmania and mass culture it. Then we will use double-photo inactivation system to completely remove its infectiousness. Repeat the same process and we can design and produce different antigen specific leijuvant.


Sponsor
We will solicit cooperation with pharmaceutical companies that produce vaccines and adjuvants, such as GSK, Merck, Novartis, Pfizer and Sanofi. Project could be improved and process more smoothly toward discussion that combine both scientific and business perception.