Ljubljana/summary

From 2007.igem.org

< Ljubljana(Difference between revisions)

Latest revision as of 18:53, 23 November 2007

Company Name

Achievements

Design and implementation of three functional systems of activation of anti-HIV defense based on:

- detection of viral interactions with the cells and
- cleavage of specific substrate by viral protease.
Successful detection of CD4-CCR5 heterodimer formation through:

- split tobacco etch virus (TEV) protease,
- split ubiquitin system.
Construction of BioBricks for heterodimerization, which represents a powerful platform for engineering cell processes based on protein-protein interactions.
Introduction of a versatile amplification platform based on the use of T7 RNA polymerase in mammalian cells.
Activation device based on the proteolytic cleavage and release of membrane-anchored T7 RNA polymerase from the membrane into the cell nucleus.
Anchoring of T7 RNA polymerase to the plasma membrane either by:

- fusion to CD4 or
- addition of a myristoylation signal.
Implementation of two different types of effector molecules for:

- induction of cell death (caspase-3) or
- activation of antiviral defense (interferon beta).
Preparation of a 12-pages brochure on Synthetic Biology aimed at high school students and general audience.

Prospects for future work and real world applications

The idea of relying on viral functions could be applied also to other HIV-specific processes (such as genome integration, reverse transcription…).
Our system based on BioBricks has been useful to prove the principle, but for the real application cellular delivery would be much better applied using vectors based on viral delivery.
In the case of using viral vectors, therapy could be targeted specifically to cells that can be infected by HIV-1 (e.g. similar to T-cell-directed retroviral delivery systems described by David Baltimore at SB2.0).
Selection of different effectors will (and can) be made based on further experiments – apoptosis can only be used in 100% leak-proof systems, while antiviral and immune response effectors are not as sensitive.
Similar systems can be prepared for therapy of many other pathogens, particularly viruses (e.g. yellow fever, SARS, foot and mouth disease…) which contain specific proteases and rely on defined cellular receptors.

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 <title>Company Name</title>
 <meta http-equiv="Content-Type" content="text/html; charset=iso-8859-1" />
-<link href="http://rokgaber.3host.biz/stylenew_zadaj.css" rel="stylesheet" type="text/css" />
+<link rel="stylesheet" href="/igem07/index.php?title=User:RGaber/stylesheet/stylenew_zadaj.css&action=raw&ctype=text/css" type="text/css" />
 </head>
 <body>
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-   <div id="supportingText">
+   <div align="justify" id="supportingText">
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    <li>Design and implementation of three functional systems of activation of anti-HIV defense based on:
     <dl>
-     <dd>- the detection of viral interactions with the cells and
+     <dd>- detection of viral interactions with the cells and
      <dd>- cleavage of specific substrate by viral protease.
     </dl>
@@ Line 44: / Line 44: @@
      <dd>- split ubiquitin system.
     </dl>
-   <li>Construction of <a href="https://2007.igem.org/Ljubljana/biobricks">BioBricks</a> for heterodimerization, which represent a powerful platform for engineering cell processes based on protein-protein interactions.
+   <li>Construction of <a href="https://2007.igem.org/Ljubljana/biobricks">BioBricks</a> for heterodimerization, which represents a powerful platform for engineering cell processes based on protein-protein interactions.
-   <li>Introduction of the versatile amplification platform based on the use of T7 RNA polymerase in mammalian cells.
+   <li>Introduction of a versatile amplification platform based on the use of T7 RNA polymerase in mammalian cells.
-   <li>Activation device based on the proteolytic cleavage and release of membrane anchored T7 RNA polymerase from the membrane into the cell nucleus.
+   <li>Activation device based on the proteolytic cleavage and release of membrane-anchored T7 RNA polymerase from the membrane into the cell nucleus.
    <li>Anchoring of T7 RNA polymerase to the plasma membrane either by:
     <dl>
@@ Line 54: / Line 54: @@
    <li>Implementation of two different types of effector molecules for:
     <dl>
-     <dd>- induction of cell death (caspase-3)or
+     <dd>- induction of cell death (caspase-3) or
      <dd>- activation of antiviral defense (interferon beta).
+   </dl><br>
+  <li>Preparation of a 12-pages <a href="https://static.igem.org/mediawiki/2007/9/99/BrochureSB07_LJU_TitlePage.jpg">brochure on Synthetic Biology</a> aimed at high school students and general audience.
     </dl>
 </ul>
@@ Line 70: / Line 72: @@
-       <h3><span>Prospects for the future work and real world applications</span></h3>
+       <h3><span>Prospects for future work and real world applications</span></h3>
        <p class="p1">
@@ Line 76: / Line 78: @@
 <ul>
 <li>The idea of relying on viral functions could be applied also to other HIV-specific processes (such as genome integration, reverse transcription…).
-<li>Our system based on <a href="https://2007.igem.org/Ljubljana/biobricks">BioBricks</a> has been useful for the proof the principle, but for the real application cellular delivery would be much better applied using vectors based on viral delivery.
+<li>Our system based on <a href="https://2007.igem.org/Ljubljana/biobricks">BioBricks</a> has been useful to prove the principle, but for the real application cellular delivery would be much better applied using vectors based on viral delivery.
-<li>In case of using viral vectors therapy could be delivered specifically to the relevant cells that can be infected by HIV-1 (e.g. similar as T-cell-directed retroviral delivery systems described by David Baltimore at SB2.0).
+<li>In the case of using viral vectors, therapy could be targeted specifically to cells that can be infected by HIV-1 (e.g. similar to T-cell-directed retroviral delivery systems described by David Baltimore at SB2.0).
 <li>Selection of different effectors will (and can) be made based on further experiments – apoptosis can only be used in 100% leak-proof systems, while antiviral and immune response effectors are not as sensitive.
-<li>Similar systems can be prepared for therapy of many other pathogens, particularly viruses (e.g. yellow fiver, SARS, foot and mouth disease…) which contain specific proteases and rely on defined cellular receptors.
+<li>Similar systems can be prepared for therapy of many other pathogens, particularly viruses (e.g. yellow fever, SARS, foot and mouth disease…) which contain specific proteases and rely on defined cellular receptors.
 </ul>
@@ Line 90: / Line 92: @@
      <div id="footer">______________________________________<br />
+<a href="https://2007.igem.org/Ljubljana/methods">Methods</a>
 |<a href="https://2007.igem.org/Ljubljana">Home</a>|
-<a href="https://2007.igem.org/Ljubljana/HIVbacground">HIV-1 Infection Background</a>
+<a href="https://2007.igem.org/Ljubljana/team">Team</a>
 </div>
    </div>
    <div id="linkList">
      <div id="linkList2">
        <div id="lmenu">
+<center>
+<a href="https://2007.igem.org/Ljubljana">
+<img border="0" src="https://static.igem.org/mediawiki/2007/c/c6/BlurMetalHome.gif" width="34" height="34">
+</center>
          <h3 class="menu"><span><a class="two" href="https://2007.igem.org/Ljubljana/AIDSplague">AIDS - Today's Plague</a></span></h3>
          <ul>
+          <li><a class="one" href="https://2007.igem.org/Ljubljana/AIDSplague">Epidemics</a>&nbsp; </li>
            <li><a class="one" href="https://2007.igem.org/Ljubljana/HIVbacground">HIV-1 Infection Background</a>&nbsp; </li>
            <li><a class="one" href="https://2007.igem.org/Ljubljana/Currenttreatment">Current Disease Treatment</a>&nbsp; </li>
@@ Line 106: / Line 116: @@
        </div>
        <div id="llinks">
-         <h3 class="links"><span><a class="two" href="https://2007.igem.org/Ljubljana/Strategy">Strategy</a></span></h3>
+         <h3 class="links"><span><a class="two" href="https://2007.igem.org/Ljubljana/Strategy">Project</a></span></h3>
          <ul>
-          <li><a class="one" href="https://2007.igem.org/Ljubljana/implementation">Implementation</a>&nbsp; </li>
+        <li><a class="one" href="https://2007.igem.org/Ljubljana/Strategy">Strategy</a>&nbsp; </li>
+<li><a class="one" href="https://2007.igem.org/Ljubljana/implementation">Implementation</a>&nbsp; </li>
            <li><a class="one" href="https://2007.igem.org/Ljubljana/model">Model</a>&nbsp; </li>
          </ul>
@@ Line 126: / Line 137: @@
          <ul>
-           <li><a class="one" href="https://2007.igem.org/Ljubljana/achievements">Achievements</a>&nbsp; </li>
+           <li><a class="one" href="https://2007.igem.org/Ljubljana/summary">Achievements</a>&nbsp; </li>
-           <li><a class="one" href="https://2007.igem.org/Ljubljana/prospects">Prospects</a>&nbsp; </li>
+           <li><a class="one" href="https://2007.igem.org/Ljubljana/summary">Prospects</a>&nbsp; </li>
@@ Line 135: / Line 146: @@
 <div id="ldiscussion">
          <h3 class="discussion"><span><a class="two" href="https://2007.igem.org/Ljubljana/team">Team</a></span></h3>
-         <ul>
+         <br><br>
+</div>
-<br><br>
-<li><a class="one" href="https://2007.igem.org/Ljubljana/glossary">Terms & References</a>&nbsp; </li>
+<div id="ldiscussion">
+<ul><li><a class="one" href="https://2007.igem.org/Ljubljana/glossary">Glossary & References</a>&nbsp; </li>
 <li><a class="one" href="https://2007.igem.org/Ljubljana/acknowledgements">Acknowledgements</a>&nbsp; </li>
           </ul>

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Ljubljana/summary

From 2007.igem.org

Latest revision as of 18:53, 23 November 2007

Achievements

Prospects for future work and real world applications

AIDS - Today's Plague

Project

Results

Summary

Team