Team:Peking/Modeling/Luminesensor

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Summary

We have managed to conduct a series of modeling simulations to guide the optimization of our Luminesensor, combining protein kinetics, thermodynamics, and stochastic simulation with molecular docking together. The modeling results point out two critical mutation sites (74 & 135) on VVD, the dimerization domain and a mutant choise of LexA, the DNA binding domain of our Luminesensor. The modeling results also shows the system still works well even if considering noise and endogenous competition.

Kinetic Network

Firstly we established a reaction network for the DNA binding process of the Luminesensor (For details see Project Luminesensor Design). Previous works by other scientists indicate that the Vivid (VVD) protein, the sensing domain of the Luminesensor, dimerizes in the presence of light,[1] and the LexA protein, the binding domain of the Luminesensor, binds at specific sequences on DNA predominantly when coupled[2] and subsequently represses the interest gene. By combining with the mechanisms of the two functional domains of the Luminesensor, we concluded with the following kinetic network (Figure 1):

Network System Fig

Figure 1. Kinetic Network of our Luminesensor

where

  • L : Luminesensor,
  • LG : the ground state --- with its VVD N-cap locked,
  • LA : the active state --- with its VVD N-cap released,
  • DL : the specific DNA binding site to Luminesensor.

Since no multi-intermediate reactions are hidden in the network above, all reactions can be regarded as elementary reactions.

Reference

  • 1. Zoltowski, B.D., Crane, B.R.(2008)Light Activation of the LOV Protein Vivid Generates a Rapidly Exchanging Dimer.Biochemistry, 47: 7012: 7019
  • 2. Mohana-Borges, R., Pacheco, A.B., Sousa, F.J., Foguel, D., Almeida, D.F., and Silva, J.L. (2000). LexA repressor forms stable dimers in solution. The role of specific DNA in tightening protein-protein interactions. J. Biol. Chem., 275: 4708: 4712
  • Totop Totop