Abstract

Translation speed can affect the cotranslational folding of nascent peptide. Experimental observations have indicated that slowing down translation rates of codons can increase the probability of protein cotranslational folding. Recently, a kinetic modeling indicates that fast translation can also increase the probability of cotranslational protein folding by avoiding misfolded intermediates. We show that the villin headpiece subdomain HP35 is an ideal model to demonstrate this phenomenon. We studied cotranslational folding of HP35 with different fast translation speeds by all-atom molecular dynamics simulations and found that HP35 can fold along a well-defined pathway that passes the on-pathway intermediate but avoids the misfolded off-pathway intermediate in certain case. This greatly increases the probability of HP35 cotranslational folding and the approximate mean first passage time of folding into native state is about 1.67μs. Since we also considered the space-confined effect of the ribosomal exit tunnel on the cotranslational folding, our simulation results suggested alternative mechanism for the increasing of cotranslational folding probability by fast translation speed.

Highlights

  • Its stability non-monotonically changes with nascent chain length

  • HP35 is an ideal model to see if fast translation can avoid the misfolded off-pathway intermediate during cotranslational folding

  • The cotranslational folding of HP35 is simulated in three steps: (1) folding in the ribosomal exit tunnel, (2) co-releasing folding from the tunnel and (3) free folding in bulk

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Summary

Introduction

Its stability non-monotonically changes with nascent chain length. HP35 is an ideal model to see if fast translation can avoid the misfolded off-pathway intermediate during cotranslational folding. In the first step of the simulations, HP35 folds starting from an extended conformation in a model of the ribosomal exit tunnel.

Results
Conclusion
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