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Caspase-Based Fusion Protein Technology: Substrate Cleavability Described by Computational Modeling and Simulation.

Jakob LiuAndreas FischerMonika Cserjan-PuschmannNico LinggChris Oostenbrink
Published in: Journal of chemical information and modeling (2024)
The Caspase-based fusion protein technology (CASPON) allows for universal cleavage of fusion tags from proteins of interest to reconstitute the native N-terminus. While the CASPON enzyme has been optimized to be promiscuous against a diversity of N-terminal peptides, the cleavage efficacy for larger proteins can be surprisingly low. We develop an efficient means to rationalize and predict the cleavage efficiency based on a structural representation of the intrinsically disordered N-terminal peptides and their putative interactions with the CASPON enzyme. The number of favorably interacting N-terminal conformations shows a very good agreement with the experimentally observed cleavage efficiency, in agreement with a conformational selection model. The method relies on computationally cheap molecular dynamics simulations to efficiently generate a diverse collection of N-terminal conformations, followed by a simple fitting procedure into the CASPON enzyme. It can be readily used to assess the CASPON cleavability a priori.
Keyphrases
  • molecular dynamics simulations
  • dna binding
  • cell death
  • molecular docking
  • amino acid
  • transcription factor
  • molecular dynamics
  • minimally invasive
  • single molecule
  • oxidative stress