Revision as of 12:31, 27 October 2008

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Introduction

The dimerization of the extracellular receptor domains is a important necessity for the functionality of our modular receptor system. Presenting the system a stimulus in the form of spatial arranged ligands, the extracellular domains dimerize, thus the corresponding intracellular parts such as the split lactamase halves or split fluorescent proteins complement to measureable output. To analyse the theoretical functionality due to dimerization, first two receptor dimerization models (one T cell receptor model and one general receptor model) are introduced and discussed and then a proper model for the modular receptor system is constructed.

T cell receptor dimerization model I

T cells are a special type of white blood cells (lymphocytes) and play a central role in cell-mediated immunity. They carry special receptors, so called T cell receptors (TCR) on their membrane. One part of the mechanisms to activate a TCR and thus to activate a T Cell is the binding of a ligand, also called antigen, to the TCR. As research showed, one single ligand-TCR complex does not lead to a T cell response yet, as at least two ligand-TCR complexes and their dimerization seem to be required for proper T cell activation (Schamel, 2006; Bachmann 1999). In our case the ligands are nitro-iodo-phenol (NIP) molecules attached to a DNA-Origami structure at a (variable) distance of ~6nm to each other. These NIPs are recognized and bound by the TCRs. As the distance is small enough for two TCRs to approach very closely when each of them binds a NIP, they can dimerize.

Extracellular signaling

A simplified pathway shows the extracellular sequence of TCR activation. After the NIP binding two complexes come together and form a dimer which then leads to activaton of the TCR and further intracellular signaling and T cell activation.

Pathway of TCR dimerization

Reaction kinetics

The T cell maintains a pool of TCRs (T) which is dynamic. The continuous de novo expression, random internalization and degradation runs with constant rate S :
200px

One NIP molecule (N) binds to a TCR (T) with the reaction rate k_on or a TCR-NIP complex (TN) dissociates with the reaction rate k_off :

250px

Two TCR-NIP (TN) complexes dimerize to a TCR-NIP dimer (TND) with rate k_don ; the dissociation of a TCR-NIP dimer runs with rate k_doff :
295px

In order to get active TCRs, the TCR-NIP dimer (TND) has to switch into two active TCRs (A) with rate k_a :
250px

After activation, the TCR is internalised with rate k_i and does not take part anymore in the extracellular signaling :
150px

@@ Line 28: / Line 28: @@
 </tr>
 </table>
+<br>
+<h3> Reaction kinetics </h3>
+<br>
+The T cell maintains a pool of TCRs ('''T''') which is dynamic. The continuous de novo expression, random internalization and degradation runs with constant rate '''S''' :
+<br>
+[[Image:Freiburg08_T_turn.png|200px]]
+<br><br>
+One NIP molecule ('''N''') binds to a TCR ('''T''') with the reaction rate '''k'''<sub>on</sub> or a TCR-NIP complex ('''TN''') dissociates with the reaction rate '''k'''<sub>off</sub> :
+<br>
+[[Image:Freiburg_08_TN_Bind2.png|250px]]
+<br><br>
+Two TCR-NIP ('''TN''') complexes dimerize to a TCR-NIP dimer ('''TND''') with rate '''k'''<sub>don</sub> ; the dissociation of a TCR-NIP dimer runs with rate '''k'''<sub>doff</sub> :
+<br>
+[[Image:Freiburg_08_TN_Dimerization2.png|295px]]
+<br><br>
+In order to get active TCRs, the TCR-NIP dimer ('''TND''') has to switch into two active TCRs ('''A''') with rate '''k'''<sub>a</sub> :
+<br>
+[[Image:Freiburg_08_active_TCR.png|250px]]
+<br><br>
+After activation, the TCR is internalised with rate '''k'''<sub>i</sub> and does not take part anymore in the extracellular signaling :
+<br>
+[[Image:Freiburg_08_TCR_i.png|150px]]
+<br><br>
 }}

Team:Freiburg/Modeling

From 2008.igem.org

Revision as of 12:31, 27 October 2008

Introduction

Contents

T cell receptor dimerization model I

Extracellular signaling

Reaction kinetics