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A Process Model of Rho GTPbinding Proteins

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A Process Model of. Rho GTP-binding Proteins. Luca Cardelli 1, 4 Emmanuelle Caron 2, 4. Philippa Gardner 3, 4 Ozan Kahramanogullari 3, 4 Andrew Phillips 1 ... – PowerPoint PPT presentation

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Title: A Process Model of Rho GTPbinding Proteins


1
A Process Model of Rho GTP-binding Proteins
  • Luca Cardelli 1, 4 Emmanuelle Caron 2,
    4
  • Philippa Gardner 3, 4 Ozan Kahramanogullari
    3, 4 Andrew Phillips 1
  • 1. Microsoft Research Cambridge
  • 2. Centre for Molecular Biology and Infection,
    Imperial College
  • 3. Department of Computing, Imperial College
  • 4. CISBIC, Imperial College
  • 20.11.2007 CISB07, Newcastle

2
Overview
  • Why Rho GTP-binding proteins?
  • Why a process model?
  • What are we doing?
  • How are we doing?
  • Outlook

3
Modelling FcR-mediated phagocytosis
Opsinized particle binds Fc Receptor. Src is
activated.
Src phosphorylates two tyrosine residues on ITAM,
which then recruits Syk-kinase.
Active Syk recruits Vav and activates it.
Vav activates Rac. Cdc42 gets activated
(somehow).
4
Cdc42 and Rac are Rho GTP-binding proteins
Etienne-Manneville Hall. Nature 2002
Rho GTP-binding proteins serve as switches that
interact with their environment. GEF and GAP
are their regulators.
5
Overview
  • Why Rho GTP-binding proteins?
  • Why a process model?
  • What are we doing?
  • How are we doing?
  • Outlook

6
Why a process model?
  • Process algebra used to study complex reactive
    systems
  • Rich arsenal of mathematical techniques and tools
    available
  • Biological systems process information
    concurrent, reactive
  • Complexation can be easily modeled, e.g., actin
    polymerization.
  • Process algebra allow modular building of
    mechanistic models.
  • Compositionality

7
Overview
  • Why Rho GTP-binding proteins?
  • Why a process model?
  • What are we doing?
  • How are we doing?
  • Outlook

8
An ODE model of Rho GTP-binding Proteins
9
Overview
  • Why Rho GTP-binding proteins?
  • Why a process model?
  • What are we doing?
  • How are we doing?
  • Outlook

10
Biological Processes as Computations
11
Rho GTP-binding Proteins with GEF and without GAP
Rho GTP-binding Proteins with GEF and without GAP
12
Rho GTP-Binding Proteins with GEF and GAP
13
Extending the Model with GDIs
14
Parameter analysis for the extended model
We vary the parameters of the processes for 4 GDI
reactions between 10-4,,104.
r1 1, r2 1 r1 104, r2 104 r1
104, r2 1 r1 104, r2 10-4 r11,
r2 10-4
and with varying r3 and r4, there is no effect on
the inhibitory behavior of the GDIs.

r11, r2104
r110-4, r2104
r110-4, r210-4
15
Outlook
  • A process model of Rho GTP-binding proteins.
  • Our model successfully mimics the ODE model.
  • We compositionally extend the model with GDIs.
  • Parameter estimation by hand (and automated?).
  • Rho GTP-binding proteins experimental validation
    of GDI and active Rho binding.
  • By composing this model with other components of
    FcR-mediated phagocytosis, e.g., actin
    polymerisation, obtain a systems understanding.
  • Reuse the Rho-GTP model as a template for Ras
    super-family proteins.

16
Acknowledgements
  • Jaroslav Stark
  • George Tzircotis
  • Jeroen van Zon
  • Simon Moon
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