Difference between revisions of "Team:Tongji China/Integrated"

 
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<br><br><br>
 
<br><br><br>
<font color="#C66C63" size="5" face="courier">
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<font color="#C66C63" size="5" face="Comic Sans MS">
 
<center><b>& BLOCK 1 &  Background Research</b></center>
 
<center><b>& BLOCK 1 &  Background Research</b></center>
 
</font>
 
</font>
<center><i><font size="4" face="courier">(Where the dream starts)</font></i></center>
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<center><i><font size="4" face="Comic Sans MS">(Where the dream starts)</font></i></center>
<br><br> In recent years, multiple ways of immunotherapy arise which leads to brand-new hope for patients with cancers and arouse our great interest to make further research. However, based on the clinical results of those like CAR-T, side effects happen with its unsteady curative effect. Improvement is needed and we are willing to take over this challenge.
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<br><br> In recent years, multiple ways of immunotherapy arise which leads to brand-new hope for patients with cancers and arouses our interest greatly to make further research. However, based on the clinical results of those like CAR-T, side effects happen as well as its unsteady curative effect. Improvement is needed and we are willing to take over this challenge.
  
<br><br>Besides, this year unexpected scandals happened in Jilin-based Changsheng Biotechnology which has been ordered by the Chinese government to cease production of its fake rabies vaccine. It brings about great influence among society and gives rise to attention and debates of vaccine production. We are fully surprised by this scandal and reflect a lot. This issue about vaccine also plays a role in leading us to determine what we what to do to make a better world.
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<br><br> Besides, this year an unexpected scandal happened in Jilin-based Changsheng Biotechnology which had been ordered by the Chinese government to cease production of its fake rabies vaccine. It brought about great influence among society and gave rise to attention and debates on vaccine production. We were fully surprised by this scandal and reflected a lot. In addition, the movie <I’m not the god of medicine> in China also reflected serious contradiction between patients and pharmaceutical factory among the cost of medicine(Shown in following video). Those issues played a role in leading us to determine what we want to do to make a better world.
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<div width="50%" height="50%">
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<p style="text-align:center"><video controls poster="https://static.igem.org/mediawiki/2018/5/5c/T--Tongji_China--picture-videoposter-1.jpg" style="position:relative"  width="80%" height="80%" >
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<source src="https://static.igem.org/mediawiki/2018/f/fe/T--Tongji_China--Dying_for_survival.mp4" type="video/mp4">
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</source></video></p></div>
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<br><br>After plenty of research and design, we set up our project based on one specific system – Type III secretion system (T3SS) and developed our goal of designing it as an antigen delivering agent for immunotherapy, which was also promising in individualized treatment. Our primary thought was rough and urgent to fill up the blank, therefore research from both professional and social field were required.
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<br><br><br><br>
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<font color="#C66C63" size="5" face="Comic Sans MS">
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<center><b>& BLOCK 2 &  Interviews for Promotion</b></center>
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</font>
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<center><i><font size="4" face="Comic Sans MS">(a Q&A journey, pursuing for being better)</font></i></center>
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<br><br><br>
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<b><font color="#EEC778" size="4" face="Comic Sans MS" weight="600"><center>*** expert in bacteria immunity – Problems solving in bacterial immunity***</center></font></b>
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<br> Though we could construct the major part of our project through self-searching on the internet and literature reading, there were some questions and negligible aspects when it came to practical application and it was of great benefit if we could get advice from professional consultant. Therefore, we invited Professor Xin Du to assist us in aspect of bacterial immunity and possibility of bringing our project into practical medicine.
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<br><br>
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<div class="prof">
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<center><b>Biography of Dr. Xin Du (杜新)</b></center><br>
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<img src="https://static.igem.org/mediawiki/2018/f/f7/T--Tongji_China--picture-hp-duxin.png" width="25%" />
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Dr. Xin Du (杜新) is a regulatory professional with unique combination of FDA and industry regulatory experience as well as international regulation knowledge and experience. He obtained his Ph.D degree from the University of Florida and completed his post-doctoral training at the National Institute of Health (NIH).  He worked for US FDA, and pharmaceutical companies of Aventis-Pastuer, Wyeth, Novartis, BMS, NPS, Actinium and Advaxis.  Currently, he is the Senior VP of Regulatory and Quality at Adlai Nortye USA Inc.  He is an Executive Council member of SAPA.
  
<br><br>After plenty of research and design, we set up our project based on one specific system – Type III secretion system (T3SS) and developed our goal of design it as an antigen delivering agent for immunotherapy, which is promising in individualized treatment. Our primary thought is rough and is necessary to fill up the blank, therefore research from both professional and social field are required.
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</div>
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<br>We prepared several questions for Dr. Du, and had a conversation with him based on these questions.
 
<br><br>
 
<br><br>
<font color="#C66C63" size="5" face="courier">
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<font face="Comic Sans MS" color="#C66C63"><b>1) About oral administration:<br></b></font><br>
<center><b>& BLOCK 2 &  Interviews for Promotion</b></center>
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Dr. Du advised that the practical aspects were how to protect the orally administrated medicines from being digested or destroyed when the medicines went through the digestion system, and how to ensure the antigens could be delivered to the targets.  Dr. Du recommended us to complete our project's focus on these important aspects.<br><br>
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<div class="people"><img src="https://static.igem.org/mediawiki/2018/4/4e/T--Tongji_China--picture--lianjie_xiaoren.jpg" width="7%" /><b><font color="#395482">→ Response:</font></b><I> we solved this by coating our bacterial with capsule.</I></div>
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<br><br>
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<font face="Comic Sans MS" color="#C66C63"><b><font face="Comic Sans MS" color="#C66C63"><b>2) Advantages in bacterial immunity compared to antigen-immunity<br></b></font></b><br>
 
</font>
 
</font>
<center><i><font size="4" face="courier">(a Q&A journey, pursuing for being better)</font></i></center>
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Dr. Du stated several advantages of bacterial immunotherapy. Firstly, the immune response by bacteria-based products could appear immediately; secondly, the antigens carried by bacterial immunotherapy products could be designed more specific to target specific cancer; Thirdly, the antigens carried by bacterial immunotherapy products were less likely to be degraded; Thus, Dr. Du was very supportive to our research project.<br><br>
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<div class="people"><img src="https://static.igem.org/mediawiki/2018/4/4e/T--Tongji_China--picture--lianjie_xiaoren.jpg" width="7%" /><b><font color="#395482">→ Response:</font></b> <I>to know the bright future of bacterial immunity really encourages us to keep moving forward.</I></div>
 
<br><br>
 
<br><br>
<b><font color="#EEC778" size="5" face="courier"><center>*** expert in bacteria immunity Problems solving in bacterial immunity***</center></font></b>
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<font face="Comic Sans MS" color="#C66C63"><b>3) Side effect in over-reactive bacterial immunotherapy products?<br></b></font><br>
 +
Like the CAR-T products, bacterial immunotherapy products could cause side effects, such as cytokine storm. To some extent, this type of side effects is an indication of that the products are working. To handle such side effects, there are co-medicines that can be used to reduce or control the side effects. Therefore, “Some of the risks are a part of the response mechanism of the bacterial immunotherapy products. The important thing we need to take care are, first, how to reduce the risks, second, if it happens, what medicine we could use to control the risks”.<br><br>
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<div class="people"><img src="https://static.igem.org/mediawiki/2018/4/4e/T--Tongji_China--picture--lianjie_xiaoren.jpg"  width="7%" /><b><font color="#395482">→ Response:</font></b><I>  It brought up our attention in such possible side effects and we did more research later. We were confirmed that there was less possibility in side effects from our production. Even if there are such side effect, there are also existing solutions to handle them.</I></div>
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<br><br>
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<font face="color="#C66C63"><b><font face="Comic Sans MS" color="#C66C63"><b>4) Clearance of exogenous bacteria.<br></b></font></b>
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</font><br>
 +
As is mentioned by Dr. Du, human body has its natural mechanism to clear the exogenous bacteria.  In addition, to ensure the full clearance of the exogenous bacteria, antibiotics are used in the clinical trials when such bacterial immunotherapies are used.<br><br>
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<div class="people"><img src="https://static.igem.org/mediawiki/2018/4/4e/T--Tongji_China--picture--lianjie_xiaoren.jpg"  width="7%" /><b><font color="#395482">→ Response:</font></b> <I>We decide to obey the rule of this “parallel protections” and design a light-control suicide system inside our bacterial.</I></div>
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<br><br>
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<font face="Comic Sans MS" color="#C66C63"><b>5) Encouragement<br></b></font><br>
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“To be or not to be, that may not be your chief question; the key is to identify the problem and find pathway to solve it.”
 +
<br>Apart from those main points to the design, Professor Du also makes significant advice on experimental designing which is of great use.
 +
<br><br><br><br>
 +
<b><font color="#EEC778" size="4" face="Comic Sans MS" weight="600"><center>*** professor in Type III secretion system instruction on the usage of tool ***</center></font></b>
 
<br>
 
<br>
<br> Though we could construct the major part of our project through self-searching on the internet and literature reading, there are some questions and negligible aspects when it comes to practical application and it is of great benefit if we could get advice from professional consultant. Therefore, we invited Professor Du Xin to assist us in aspect of bacterial immunity and possibility of bringing our project into practical medicine.
+
We learned through research that the <I>P. aeruginosa</I> has certain invasive ability, which means they will invade the cells, and eventually enter the blood after oral administration. We concerned about the safety issue on <I>P. aeruginosa</I> and its advantages over <I>Salmonella</I> and <I>Yersinia</I>, therefore, professional instructions of using <I>P. aeruginosa</I> orally is necessary.<br><br>
<br>
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<div class="prof">
<img src="img/T--Tongji_China--background.png">
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<center><b>Biography of Dr. Fang Bai (白芳)</b></center><br>
<div class="instructionOfPicture">
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<img src="https://static.igem.org/mediawiki/2018/f/f8/T--Tongji_China--picture--Dr_Fangbai.jpg" width="200" height="250"/>
Professor Du
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Fang Bai (白芳), Associate Professor, School of Pharmacy, Nankai University,  focusing on microbial and biochemical
 +
drugs and making great progress in utilizing <I>P. aeruginosa</I> Type III secretion system to deliver transcription factors to achieve the gene editing of PSCs and to trigger differentiation of ESCs. Also professional at the treatment of <I>P. aeruginosa</I> infection.<br><br><br><br>
 
</div>
 
</div>
<br><br> We concluded the conversation into several tips we got as inspiration and project promotion:
 
 
<br>
 
<br>
<font face="courier" color="#C66C63"><b>1) About oral administration:<br></b></font>
 
Professor raised the questions like -- “Questions are that how to protect your medicine from digesting when being taken orally and how to achieve the antigen-presentation on target……” and instruct us to complete our projects based on those.
 
<center><b><font color="#395482">→ Response:</font></b> we solve this by coating our bacterial with capsule.</center>
 
<br>
 
<font face="courier" color="#C66C63"><b><font face="courier" color="#C66C63"><b>2) Advantages in bacterial immunity compared to antigen-immunity<br></b></font><br></b>
 
</font>
 
Professor Du provided several advantages from bacterial immunity. Firstly, the immunoreaction could appear immediately, basically faster than antigen-immunity; secondly the antigens could be designed more specific to trigger the immunity; Thirdly, with the protection of the cell body the antigen is less likely to be degraded; Fourthly, research revealed that bacterial immunity shows evidence in on-target reaction, which is promising for cancer therapy. Therefore, Professor Du is optimistic to our idea.
 
<center><b><font color="#395482">→ Response:</font></b> to know the bright future of bacterial immunity really encourages us to keep moving forward.</center>
 
<br>
 
<font face="courier" color="#C66C63"><b>3) Side effect in over-triggering the immunity?<br></b></font>
 
Professor Du propose to take CAR-T as an example. To some extent, functions are confirmed only through detecting of those side effects, such as cytokine storm. However, there are co-medicine to reduce the bad influence from those side effects. Therefore, “Some of the risk are part of the response mechanism, but the thing we need to take care is, first, how to reduce it, second, if it happens, what medicine we could use to handle it”.
 
<center><b><font color="#395482">→ Response:</font></b> It arises our attention in this possible side effects and we did some research later. We are confirmed that there is less possibility in side effects from our production. Even if there is one side effect, there is also one existing solution to treat.</center>
 
<br>
 
<font face="color="#C66C63"><b><font face="courier" color="#C66C63"><b>4) Clearage of exogenous bacterial after effect?<br></b></font><br></b>
 
</font>
 
As is mentioned by Professor Du, there is natural mechanism of clearage in vivo, which plays a major rule in the clearage of exogenous bacterial. Besides, antibiotics are recommended in clinical therapy. With both protection methods, it is guaranteed that the engineered bacterial could be cleaned thoroughly after their effects.
 
<center><b><font color="#395482">→ Response:</font></b> We decide to obey the rule of this “parallel protections” and design a light-control suicide system inside our bacterial.</center>
 
<br>
 
<font face="courier" color="#C66C63"><b><font face="courier" color="#C66C63"><b>5) Encouragement<br></b></font><br></b>
 
</font>
 
“To be or not to be, that may not be your chief question; the key is to identify the problem and find pathway to solve it.”
 
<br><br> Apart from those main points for the design, Professor Du also makes significant advice in experimental designing which is of great use.
 
<br><br>
 
<b><font color="#EEC778" size="4" face="courier" style="white-space: nowrap;"><center>*** professor in Type III secretion system – instruction on the usage of tool ***</center></font></b>
 
<br>
 
<br>
 
We learned through researches that the P. aeruginosa has certain invasive ability, which means they will invade the cells, and eventually enter the blood after oral administration. We concerned about the safety issue about P. aeruginosa and its advantages over Salmonella and Yersinia, therefore, professional instruction of using P. aeruginosa orally is necessary.
 
<div class="instructionOfPicture">
 
<br><br>
 
Biography of Dr. Fang Bai
 
</div>
 
<br><br>
 
Fang Bai, Associate Professor, School of Pharmacy, Nankai University,  focusing on microbial and biochemical drugs and making a great progress in utilizing P. aeruginosa Type III secretion system to deliver transcription factors to achieve the gene editing of PSCs and to trigger diferenciation of ESCs. Also professional at the threatment of P. aeruginosa.
 
<br><br>
 
 
We received professional instructions in the following aspects:<br>
 
We received professional instructions in the following aspects:<br>
The safety issue on P. aeruginosa<br>
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<ul>
The advantages over Salmonella and Yersinia<br>
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<li>The safety issue on <I>P. aeruginosa</I></li>
The advantages of oral administration over intravenous injection<br><br>
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<li>The advantages over <I>Salmonella</I> and <I>Yersinia</I></li>
<font face="courier" color="#C66C63"><b><font face="courier" color="#C66C63"><b>
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<li>The advantages of oral administration over intravenous injection</li>
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</ul>
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<br>
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<font face="Comic Sans MS" color="#C66C63"><b><font face="Comic Sans MS" color="#C66C63"><b>
 
Introduction1:<br></b></font><br></b>
 
Introduction1:<br></b></font><br></b>
 
</font>
 
</font>
The attenuated strain you use are auxotrophic delta 9 in which μA gene is mutated. This strain can only grow in the presence of D-type glutamate. The human body does not contain D-type glutamate. So, the P. aeruginosa will cleave when it enters the human body. Secondly, because it is oral intake, the number of bacteria in the blood will be very small. Even if the auxotrophic bacteria enter the blood, they do not have the ability to self-reproduce and do not cause infection.
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"The attenuated strain you use are auxotrophic delta 9 in which μA gene is mutated. This strain can only grow in the presence of D-type glutamate. The human body does not contain D-type glutamate. So, the <I>P. aeruginosa</I> will cleave when it enters the human body. Secondly, because it is oral intake, the number of bacteria in the blood will be very small. Even if the auxotrophic bacteria enter the blood, they do not have the ability to self-reproduce and do not cause infection."
 
<br><br>
 
<br><br>
<font face="courier" color="#C66C63"><b><font face="courier" color="#C66C63"><b>
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<font face="Comic Sans MS" color="#C66C63"><b><font face="Comic Sans MS" color="#C66C63"><b>
 
Introduction2:<br></b></font><br></b>
 
Introduction2:<br></b></font><br></b>
 
</font>
 
</font>
Salmonella can colonize in the gut and enter the intestinal epithelial cells. Studies have shown that P. aeruginosa cannot colonize in the intestine, so the time of function time of the bacteria after entering the intestine is limited. Since it is not the bacteria colonized in the intestine, the microorganisms originally present in the intestine threaten its survival, so does the immune system. In other words, the intestinal flora is the first major threat to the P. aeruginosa, followed by the intestinal immune system. Therefore, in the intestinal tract, the P. aeruginosa will be cleared a lot so using it will be relatively safe.
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"<I>Salmonella</I> can colonize in the gut and enter the intestinal epithelial cells. Studies have shown that <I>P. aeruginosa</I> cannot colonize in the intestine, so time for bacteria to work after entering the intestine is limited. Since it is not the original bacteria colonized in the intestine, the microorganisms originally present in the intestine will threaten its survival, so does the immune system. In other words, the intestinal flora is the first major threat to the <I>P. aeruginosa</I>, followed by the intestinal immune system. Therefore, in the intestinal tract, the <I>P. aeruginosa</I> will be cleared a lot so using it will be relatively safe."
 
<br>
 
<br>
One of the features of your system is the use of a Type III secretion system to inject antigens into cells. If we need to apply antigen to anti-tumor immunity, we need to activate the reaction of CD8+ T cells, which is the cytotoxic response. Therefore, these antigens must be released into the cytoplasm of antigen-presenting cells in the form of a soluble protein, which can be extracted by MHC class I molecules to activate the CD8 response. Our system of P. aeruginosa, it happens to use its type III secretion system to inject antigens into the cell, and the P. aeruginosa itself does not enter the cell.
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"One of the features of your system is the use of a Type III secretion system to inject antigens into cells. If we need to apply antigen to anti-tumor immunity, we need to activate the reaction of CD8+ T cells, which is the cytotoxic response. Therefore, these antigens must be released into the cytoplasm of antigen-presenting cells in the form of a soluble protein, which can be extracted by MHC class I molecules to activate the CD8 response. Our system of <I>P. aeruginosa</I>, it happens to use its type III secretion system to inject antigens into the cell, and the <I>P. aeruginosa</I> itself does not enter the cell."
 
<br><br>
 
<br><br>
<font face="courier" color="#C66C63"><b><font face="courier" color="#C66C63"><b>
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<font face="Comic Sans MS" color="#C66C63"><b><font face="Comic Sans MS" color="#C66C63"><b>
 
Introduction3:<br></b></font><br></b>
 
Introduction3:<br></b></font><br></b>
 
</font>
 
</font>
I think that for the treatment of cancer, if it is a solid cancer, you can actually consider the method of injection, or oral presentation through the intestines can also be a good way. About this intravenous injection you mentioned. We have also done intravenous injections experiment. After intravenous injection, P. aeruginosa is more likely to gather in two organs. One is the liver and the other is the spleen. We found that P. aeruginosa can inject proteins into the spleen's various immune cells such as parenchyma cells, neutrophils, and macrophages through the type III secretion system. So, I think for you, still do oral, the intestines are better.
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"I think that for the treatment of cancer, if it is a solid cancer, you can actually consider the method of injection. Oral presentation through the intestines can also be a good way. About this intravenous injection you mentioned. We have also done intravenous injections experiment. After intravenous injection, <I>P. aeruginosa</I> is more likely to gather in two organs. One is the liver and the other is the spleen. We found that <I>P. aeruginosa</I> can inject proteins into the spleen's various immune cells such as parenchyma cells, neutrophils, and macrophages through the type III secretion system. So, I think, for you still do oral, the intestines are better."
 
<br><br>
 
<br><br>
 
All those instructions had great effect on our following design on the project, some of which also provided support and encouragement to our idea.
 
All those instructions had great effect on our following design on the project, some of which also provided support and encouragement to our idea.
 
<br>
 
<br>
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<br><br>
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<b><font color="#EEC778" size="4" face="Comic Sans MS" weight="600"><center>*** doctor in Lung Hospital – clarify situation of immunotherapy clinically ***</center></font></b>
 
<br>
 
<br>
<b><font color="#EEC778" size="4" face="courier" style="white-space: nowrap;"><center>*** doctor in Lung Hospital – clarify situation of immunotherapy clinically ***</center></font></b>
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 +
<img src="https://static.igem.org/mediawiki/2018/8/82/T--Tongji_China--picture--Human_Practice--2.png" width="30%" style="float: right;"> For the promising application of our project to people’s health condition, it is significant to consider the actual application, possible patient responses and promote our design specifically. Therefore, we made our visit to doctors in lung cancer at Lung Hospital affiliated to Tongji University.
 +
<br><br> Here are points of view from the doctors:
 +
<br>1) Individualized Treatment of cancer would be promising in the future. Current therapy shows different effects in different clinical cases, sometimes it is confused even to doctors that whether the common therapy could work to specific patient. With the development of NGS (next generation sequencing), it would be a trend to treat patients more individualized.
 
<br>
 
<br>
 +
<br>2) The main limitation in future Individualized Treatment is the common standard for selection of antigens. Since it has already been available for a great amount of companies to do the sequencing, what matters most now will be the way to select target antigens, of which a standard for selecting is required.
 
<br>
 
<br>
<img src="https://static.igem.org/mediawiki/2018/8/82/T--Tongji_China--picture--Human_Practice--2.png" width="30%" style="float: right;"> For the promising application of our project to people’s health condition, it is significant to consider the actual application and possible patient responses and promote our design specifically. Therefore, we made our visit to a doctor Likun Hou in lung cancer at Lung Hospital affiliated to Tongji University.
+
<br>3) Possible patients’ attitude towards our product:
<br><br> Here are points of view from the doctor:
+
<br>We are concerned that whether the patient would refuse to intake our products for it depends on live bacterial-delivery. However, the doctor claimed that what patients care most is the effect of your product. As long as it has effects in curing the illness, they’d love to have a try. Take PD-1 inhibitor as an example. Despite its high expense and relative low rate for curing (around 30%), there are still patients who choose to take it. Therefore, there is no need to worry about refuses from patients’
<br>1) Individualized Treatment of cancer would be promising in future. Current therapy shows different effects in different clinical cases, sometimes it is confused even to doctors that whether the common therapy could work to specific patient. With the development of NGS (next generation sequencing), it would be a trend to treat patients more individualized.
+
 
<br>
 
<br>
<br>2) The main limitation in future Individualized Treatment is the common standard for selection of antigens. It has already been available for a great amount of companies to do the sequencing, what matters most would be the way to select target antigens, which a standard for selecting is required.
+
<br>4) Opinions on our projects:
<br>
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<br>The idea is quite interesting. First it would reduce the cost of immunotherapy, despite the fact that current research for completing this therapy would take great amount of money. Secondly, compared to current immunotherapy such as CAR-T, your project seems more safe , which may leads to less side effects. Therefore, I suppose your project has great potential.
<br>3) Possible patients’ attitude towards our products:
+
<br><br><br><br>
<br>We are concerned that whether the patient would refuse to intake our products for it depends on live bacterial-delivery. However, doctor Hou claimed that what patients care most is the effect of your product. As long as it has effects in curing the illness, they’d love to have a try. Take PD-1 inhibitor as an example. Despite its high expense and relative low rate for curing (around 30%), there are still patients choose to take it. Therefore, there is no need to worry about refuses from patients’
+
<font color="#C66C63" size="5" face="Comic Sans MS">
<br>
+
<br>4) Opinions to our projects:
+
<br>The idea is quite interesting. First it would reduce the cost of immunotherapy, despite the fact that current research for completing this therapy would take great amount of money. Secondly, It seems more safe compared to current immunotherapy such as CAR-T, which may leads to less side effects. Therefore, I suppose your project has great potentials.
+
<br><br>
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<font color="#C66C63" size="5" face="courier">
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<center><b>& BLOCK 3 &  Visit for practical production</b></center>
 
<center><b>& BLOCK 3 &  Visit for practical production</b></center>
 
</font>
 
</font>
<center><i><font size="4" face="courier">(step by step, we are closer to apply)</font></i></center>
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<center><i><font size="4" face="Comic Sans MS">(step by step, we are closer to apply)</font></i></center>
 
<br><br>
 
<br><br>
<b><font color="#EEC778" size="5" face="courier"><center>*** “Visit medicine enterprise” – find coat for our “candy” ***</center></font></b>
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<b><font color="#EEC778" size="4" face="Comic Sans MS" weight="600"><center>*** “Visit medicine enterprise” – find coat for our “candy” ***</center></font></b>
<br>To guarantee that our project would eventually develop practical medicine product for cancer therapy, we visited local pharmaceutical factory – <b>Shanghai Roche Ltd</b>. for advice in medicine capsules. After the visit of workshops for capsule coating, we were suggested that the capsule coats were available to buy in several companies, which they offered us a list to choose. Besides, they recommended that since our final products are in small amount, it was possible to acquire capsules from their recommended companies and coat our products by ourselves in the lab. Besides, they offered to assist the design of the capsules, accessory compounds adding and operation procedures for coating if was needed.
+
<br>To guarantee that our project would eventually develop practical medicine product for cancer therapy, we visited local pharmaceutical factory – <b>Shanghai Roche Ltd</b>. for advice on medicine capsules. After the visit to workshops for capsule coating, we were suggested that the capsule coats were available to buy in several companies, which they offered us a list to choose. Besides, they recommended that since our final products were in small amount, it was possible to acquire capsules from their recommended companies and coat our products by ourselves in the lab. Besides, they offered to assist the design of the capsules, accessory compounds adding and operation procedures for coating if was needed.
 
<center><img src="https://static.igem.org/mediawiki/2018/e/ec/T--Tongji_China--picture-Team-collaboration-4.jpg" width="45%">&emsp;<img src="https://static.igem.org/mediawiki/2018/b/b2/T--Tongji_China--picture-Team-collaboration-3.jpg" width="45%"></center>
 
<center><img src="https://static.igem.org/mediawiki/2018/e/ec/T--Tongji_China--picture-Team-collaboration-4.jpg" width="45%">&emsp;<img src="https://static.igem.org/mediawiki/2018/b/b2/T--Tongji_China--picture-Team-collaboration-3.jpg" width="45%"></center>
 
<center><b><font color="#395482">→ Response:</font></b> We accept their recommend for coating, which would be seen in
 
<center><b><font color="#395482">→ Response:</font></b> We accept their recommend for coating, which would be seen in
Line 133: Line 161:
 
</center>
 
</center>
 
<br><br>
 
<br><br>
<font color="#C66C63" size="5" face="courier">
+
<font color="#C66C63" size="5" face="Comic Sans MS">
 
<center><b>& BLOCK 4 &  Social Surveys</b></center>
 
<center><b>& BLOCK 4 &  Social Surveys</b></center>
 
</font>
 
</font>
<center><i><font size="4" face="courier">(open the window and open to the voice outside the lab)</font></i></center>
+
<center><i><font size="4" face="Comic Sans MS">(open the window and open to the voice outside the lab)</font></i></center>
<br><br>
+
<br><br>Tumor related questionnaire
 +
<br>In order to make our project more feasible and necessary, we conducted a tumor-related questionnaire to the society. In this way, our projects can be carried out better. We investigated three aspects of cancer treatment, cancer treatment drugs and oral bacteria. We asked people what they think about existing cancer treatments, price of cancer treatments, developing anticancer drugs in China, and oral administration of bacteria.
 +
<div width="50%" height="50%">
 +
<p style="text-align:center"><img src="https://static.igem.org/mediawiki/2018/4/43/T--Tongji_China--picture-HP-survey-0.png " width="60% "></p></div>
 +
<br>After a month of investigation, 409 people in total filled out the questionnaire, most of whom were college students and high school students. However, more than half of them have cancer patients among their relatives and friends.<br><br>
 +
<b>Age: </b><br><br>
 +
<img src="https://static.igem.org/mediawiki/2018/8/86/T--Tongji_China--picture-survey-1.png " width="100% ">
 +
<br>
 +
<b>Education background: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/5/52/T--Tongji_China--picture-survey-2.png " width="100% ">
 +
<br><br>
 +
<b>Do any of your friends or relatives have cancer: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/5/55/T--Tongji_China--picture-survey-3.png " width="100% ">
 +
 
 +
 +
 
 +
<br><br>In terms of cancer treatment, most people choose targeted drug therapy, a quarter choose surgery and radiotherapy and chemotherapy, and only a small number of people choose personalized gene therapy. In terms of problems with cancer treatment in China, most people think that the problem lies in drug prices and medical standards. More than 90% of people said that the price of cancer treatment is more expensive, and 40% of them said they could not afford it. It can be seen that the popularity of targeted drug therapy is much higher than that of gene therapy. A large part of the reason is that the cost of gene therapy is too high, and ordinary people cannot afford expensive treatment costs. Therefore, cheaper tumor therapies are urgently needed.
 +
<br><br>
 +
<b>Most acceptable ways of tumor treatment: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/d/d5/T--Tongji_China--picture-survey-4.png " width="100% ">
 +
<br><br>
 +
<b>The biggest problem facing tumor treatment in China: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/5/53/T--Tongji_China--picture-survey-5.png "width="100% ">
 +
<br><br>
 +
<b>The price of drugs for cancer treatment: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/7/7f/T--Tongji_China--picture-survey-6.png "width="100% ">
 +
 +
<br><br>For the reason that the price of drugs is too expensive, most people think that because of the huge investment in research and development, the drug price is too high. And more than half of them support China's independent research and development of new drugs or research and development of new treatments, and another one-third believe that imported drugs should be included in medical insurance, thereby reducing the price of drugs, so that more people can afford the price of cancer drugs. However, in recent years, the efficiency of China's independent research and development of new anti-tumor drugs has been very low. For this phenomenon, most people think that it is the lack of talents and the derailment of scientific research departments and pharmaceutical companies. Therefore, the cultivation of scientific research talents and the application of scientific research results are crucial for China's independent research and development of drugs.
 +
<br><br>
 +
<b>The specific reason for your opinion: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/e/e2/T--Tongji_China--picture-survey-7.png " width="100% ">
 +
<br><br>
 +
<b> The most important reason for the high price of cancer drugs may be:</b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/1/10/T--Tongji_China--picture-survey-8.png " width="100% ">
 +
<br><br>
 +
<b>The most supportive approach to addressing the high cost of cancer treatment: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/4/48/T--Tongji_China--picture-survey-9.png " width="100% ">
 +
<br><br>
 +
<b>Attitude to the independent research and development of drugs to treat tumor in China: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/1/1c/T--Tongji_China--picture-survey-10.png " width="100% ">
 +
 +
 +
<br><br>In the case of oral administration of bacteria, most people have indicated that they can accept the method of modifying the gut microbiota gene to treat diseases. But for the treatment of engineering bacteria, more than half of people prefer intravenous injection rather than oral administration. Because most people believe that oral administration can not accurately control the efficacy, at the same time, its safety is not guaranteed. However, oral bacteria may reduce unnecessary pain compared to intravenous injection. Therefore, if it comes to develop an engineered bacteria that can be taken orally, efficacy and safety must be taken into consideration.
 +
<br><br>
 +
<b>Attitude to genetically modified bacterial therapy: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/4/42/T--Tongji_China--picture-survey-11.png "width="100% ">
 +
<br><br>
 +
<b>Selection of bacterial administration methods:</b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/3/38/T--Tongji_China--picture-survey-12.png "width="100% ">
 +
<br><br>
 +
<b>Concern about oral bacteria: </b>
 +
<br><br><img src="https://static.igem.org/mediawiki/2018/c/c3/T--Tongji_China--picture-survey-13.png "width="100% ">
 +
 
 +
<br><br>From the survey above, we believe that our project should focus on developing a cheaper and safer treatment for cancer. At the same time, we need to actively apply our results to promote the development of cancer treatment in China and the world.<br><br><br>
 +
 
 
</div>
 
</div>
 
                 </div>
 
                 </div>

Latest revision as of 03:47, 18 October 2018

Integrated
Human Practice
Integrated Human Practice



& BLOCK 1 & Background Research
(Where the dream starts)


In recent years, multiple ways of immunotherapy arise which leads to brand-new hope for patients with cancers and arouses our interest greatly to make further research. However, based on the clinical results of those like CAR-T, side effects happen as well as its unsteady curative effect. Improvement is needed and we are willing to take over this challenge.

Besides, this year an unexpected scandal happened in Jilin-based Changsheng Biotechnology which had been ordered by the Chinese government to cease production of its fake rabies vaccine. It brought about great influence among society and gave rise to attention and debates on vaccine production. We were fully surprised by this scandal and reflected a lot. In addition, the movie in China also reflected serious contradiction between patients and pharmaceutical factory among the cost of medicine(Shown in following video). Those issues played a role in leading us to determine what we want to do to make a better world.



After plenty of research and design, we set up our project based on one specific system – Type III secretion system (T3SS) and developed our goal of designing it as an antigen delivering agent for immunotherapy, which was also promising in individualized treatment. Our primary thought was rough and urgent to fill up the blank, therefore research from both professional and social field were required.



& BLOCK 2 & Interviews for Promotion
(a Q&A journey, pursuing for being better)



*** expert in bacteria immunity – Problems solving in bacterial immunity***

Though we could construct the major part of our project through self-searching on the internet and literature reading, there were some questions and negligible aspects when it came to practical application and it was of great benefit if we could get advice from professional consultant. Therefore, we invited Professor Xin Du to assist us in aspect of bacterial immunity and possibility of bringing our project into practical medicine.

Biography of Dr. Xin Du (杜新)

Dr. Xin Du (杜新) is a regulatory professional with unique combination of FDA and industry regulatory experience as well as international regulation knowledge and experience. He obtained his Ph.D degree from the University of Florida and completed his post-doctoral training at the National Institute of Health (NIH). He worked for US FDA, and pharmaceutical companies of Aventis-Pastuer, Wyeth, Novartis, BMS, NPS, Actinium and Advaxis. Currently, he is the Senior VP of Regulatory and Quality at Adlai Nortye USA Inc. He is an Executive Council member of SAPA.

We prepared several questions for Dr. Du, and had a conversation with him based on these questions.

1) About oral administration:

Dr. Du advised that the practical aspects were how to protect the orally administrated medicines from being digested or destroyed when the medicines went through the digestion system, and how to ensure the antigens could be delivered to the targets. Dr. Du recommended us to complete our project's focus on these important aspects.

→ Response: we solved this by coating our bacterial with capsule.


2) Advantages in bacterial immunity compared to antigen-immunity

Dr. Du stated several advantages of bacterial immunotherapy. Firstly, the immune response by bacteria-based products could appear immediately; secondly, the antigens carried by bacterial immunotherapy products could be designed more specific to target specific cancer; Thirdly, the antigens carried by bacterial immunotherapy products were less likely to be degraded; Thus, Dr. Du was very supportive to our research project.

→ Response: to know the bright future of bacterial immunity really encourages us to keep moving forward.


3) Side effect in over-reactive bacterial immunotherapy products?

Like the CAR-T products, bacterial immunotherapy products could cause side effects, such as cytokine storm. To some extent, this type of side effects is an indication of that the products are working. To handle such side effects, there are co-medicines that can be used to reduce or control the side effects. Therefore, “Some of the risks are a part of the response mechanism of the bacterial immunotherapy products. The important thing we need to take care are, first, how to reduce the risks, second, if it happens, what medicine we could use to control the risks”.

→ Response: It brought up our attention in such possible side effects and we did more research later. We were confirmed that there was less possibility in side effects from our production. Even if there are such side effect, there are also existing solutions to handle them.


4) Clearance of exogenous bacteria.

As is mentioned by Dr. Du, human body has its natural mechanism to clear the exogenous bacteria. In addition, to ensure the full clearance of the exogenous bacteria, antibiotics are used in the clinical trials when such bacterial immunotherapies are used.

→ Response: We decide to obey the rule of this “parallel protections” and design a light-control suicide system inside our bacterial.


5) Encouragement

“To be or not to be, that may not be your chief question; the key is to identify the problem and find pathway to solve it.”
Apart from those main points to the design, Professor Du also makes significant advice on experimental designing which is of great use.



*** professor in Type III secretion system – instruction on the usage of tool ***

We learned through research that the P. aeruginosa has certain invasive ability, which means they will invade the cells, and eventually enter the blood after oral administration. We concerned about the safety issue on P. aeruginosa and its advantages over Salmonella and Yersinia, therefore, professional instructions of using P. aeruginosa orally is necessary.

Biography of Dr. Fang Bai (白芳)

Fang Bai (白芳), Associate Professor, School of Pharmacy, Nankai University, focusing on microbial and biochemical drugs and making great progress in utilizing P. aeruginosa Type III secretion system to deliver transcription factors to achieve the gene editing of PSCs and to trigger differentiation of ESCs. Also professional at the treatment of P. aeruginosa infection.




We received professional instructions in the following aspects:
  • The safety issue on P. aeruginosa
  • The advantages over Salmonella and Yersinia
  • The advantages of oral administration over intravenous injection

Introduction1:

"The attenuated strain you use are auxotrophic delta 9 in which μA gene is mutated. This strain can only grow in the presence of D-type glutamate. The human body does not contain D-type glutamate. So, the P. aeruginosa will cleave when it enters the human body. Secondly, because it is oral intake, the number of bacteria in the blood will be very small. Even if the auxotrophic bacteria enter the blood, they do not have the ability to self-reproduce and do not cause infection."

Introduction2:

"Salmonella can colonize in the gut and enter the intestinal epithelial cells. Studies have shown that P. aeruginosa cannot colonize in the intestine, so time for bacteria to work after entering the intestine is limited. Since it is not the original bacteria colonized in the intestine, the microorganisms originally present in the intestine will threaten its survival, so does the immune system. In other words, the intestinal flora is the first major threat to the P. aeruginosa, followed by the intestinal immune system. Therefore, in the intestinal tract, the P. aeruginosa will be cleared a lot so using it will be relatively safe."
"One of the features of your system is the use of a Type III secretion system to inject antigens into cells. If we need to apply antigen to anti-tumor immunity, we need to activate the reaction of CD8+ T cells, which is the cytotoxic response. Therefore, these antigens must be released into the cytoplasm of antigen-presenting cells in the form of a soluble protein, which can be extracted by MHC class I molecules to activate the CD8 response. Our system of P. aeruginosa, it happens to use its type III secretion system to inject antigens into the cell, and the P. aeruginosa itself does not enter the cell."

Introduction3:

"I think that for the treatment of cancer, if it is a solid cancer, you can actually consider the method of injection. Oral presentation through the intestines can also be a good way. About this intravenous injection you mentioned. We have also done intravenous injections experiment. After intravenous injection, P. aeruginosa is more likely to gather in two organs. One is the liver and the other is the spleen. We found that P. aeruginosa can inject proteins into the spleen's various immune cells such as parenchyma cells, neutrophils, and macrophages through the type III secretion system. So, I think, for you still do oral, the intestines are better."

All those instructions had great effect on our following design on the project, some of which also provided support and encouragement to our idea.


*** doctor in Lung Hospital – clarify situation of immunotherapy clinically ***

For the promising application of our project to people’s health condition, it is significant to consider the actual application, possible patient responses and promote our design specifically. Therefore, we made our visit to doctors in lung cancer at Lung Hospital affiliated to Tongji University.

Here are points of view from the doctors:
1) Individualized Treatment of cancer would be promising in the future. Current therapy shows different effects in different clinical cases, sometimes it is confused even to doctors that whether the common therapy could work to specific patient. With the development of NGS (next generation sequencing), it would be a trend to treat patients more individualized.

2) The main limitation in future Individualized Treatment is the common standard for selection of antigens. Since it has already been available for a great amount of companies to do the sequencing, what matters most now will be the way to select target antigens, of which a standard for selecting is required.

3) Possible patients’ attitude towards our product:
We are concerned that whether the patient would refuse to intake our products for it depends on live bacterial-delivery. However, the doctor claimed that what patients care most is the effect of your product. As long as it has effects in curing the illness, they’d love to have a try. Take PD-1 inhibitor as an example. Despite its high expense and relative low rate for curing (around 30%), there are still patients who choose to take it. Therefore, there is no need to worry about refuses from patients’

4) Opinions on our projects:
The idea is quite interesting. First it would reduce the cost of immunotherapy, despite the fact that current research for completing this therapy would take great amount of money. Secondly, compared to current immunotherapy such as CAR-T, your project seems more safe , which may leads to less side effects. Therefore, I suppose your project has great potential.



& BLOCK 3 & Visit for practical production
(step by step, we are closer to apply)


*** “Visit medicine enterprise” – find coat for our “candy” ***

To guarantee that our project would eventually develop practical medicine product for cancer therapy, we visited local pharmaceutical factory – Shanghai Roche Ltd. for advice on medicine capsules. After the visit to workshops for capsule coating, we were suggested that the capsule coats were available to buy in several companies, which they offered us a list to choose. Besides, they recommended that since our final products were in small amount, it was possible to acquire capsules from their recommended companies and coat our products by ourselves in the lab. Besides, they offered to assist the design of the capsules, accessory compounds adding and operation procedures for coating if was needed.
→ Response: We accept their recommend for coating, which would be seen in P.A.


& BLOCK 4 & Social Surveys
(open the window and open to the voice outside the lab)


Tumor related questionnaire
In order to make our project more feasible and necessary, we conducted a tumor-related questionnaire to the society. In this way, our projects can be carried out better. We investigated three aspects of cancer treatment, cancer treatment drugs and oral bacteria. We asked people what they think about existing cancer treatments, price of cancer treatments, developing anticancer drugs in China, and oral administration of bacteria.


After a month of investigation, 409 people in total filled out the questionnaire, most of whom were college students and high school students. However, more than half of them have cancer patients among their relatives and friends.

Age:


Education background:



Do any of your friends or relatives have cancer:



In terms of cancer treatment, most people choose targeted drug therapy, a quarter choose surgery and radiotherapy and chemotherapy, and only a small number of people choose personalized gene therapy. In terms of problems with cancer treatment in China, most people think that the problem lies in drug prices and medical standards. More than 90% of people said that the price of cancer treatment is more expensive, and 40% of them said they could not afford it. It can be seen that the popularity of targeted drug therapy is much higher than that of gene therapy. A large part of the reason is that the cost of gene therapy is too high, and ordinary people cannot afford expensive treatment costs. Therefore, cheaper tumor therapies are urgently needed.

Most acceptable ways of tumor treatment:



The biggest problem facing tumor treatment in China:



The price of drugs for cancer treatment:



For the reason that the price of drugs is too expensive, most people think that because of the huge investment in research and development, the drug price is too high. And more than half of them support China's independent research and development of new drugs or research and development of new treatments, and another one-third believe that imported drugs should be included in medical insurance, thereby reducing the price of drugs, so that more people can afford the price of cancer drugs. However, in recent years, the efficiency of China's independent research and development of new anti-tumor drugs has been very low. For this phenomenon, most people think that it is the lack of talents and the derailment of scientific research departments and pharmaceutical companies. Therefore, the cultivation of scientific research talents and the application of scientific research results are crucial for China's independent research and development of drugs.

The specific reason for your opinion:



The most important reason for the high price of cancer drugs may be:



The most supportive approach to addressing the high cost of cancer treatment:



Attitude to the independent research and development of drugs to treat tumor in China:



In the case of oral administration of bacteria, most people have indicated that they can accept the method of modifying the gut microbiota gene to treat diseases. But for the treatment of engineering bacteria, more than half of people prefer intravenous injection rather than oral administration. Because most people believe that oral administration can not accurately control the efficacy, at the same time, its safety is not guaranteed. However, oral bacteria may reduce unnecessary pain compared to intravenous injection. Therefore, if it comes to develop an engineered bacteria that can be taken orally, efficacy and safety must be taken into consideration.

Attitude to genetically modified bacterial therapy:



Selection of bacterial administration methods:



Concern about oral bacteria:



From the survey above, we believe that our project should focus on developing a cheaper and safer treatment for cancer. At the same time, we need to actively apply our results to promote the development of cancer treatment in China and the world.