Folding of VemP into translation-arresting secondary structure is driven by the ribosome exit tunnel
Folding of VemP into translation-arresting secondary structure is driven by the ribosome exit tunnel
Abstract The ribosome is a fundamental biomolecular complex responsible for protein production in cells. Nascent proteins emerge from the ribosome through a tunnel, where they may interact with the tunnel walls or small molecules such as antibiotics. These interactions can cause translational arrest with notable physiologic consequences. Here, we studied the arrest caused by the regulatory peptide VemP, which is known to form an α-helix in the ribosome tunnel near the peptidyl transferase center under specific conditions. We used all-atom molecular dynamics simulations of the entire ribosome and circular dichroism spectroscopy to study the driving forces of helix formation and how VemP causes the translational arrest. To that aim, we compared VemP dynamics in the ribosome tunnel with its dynamics in solution. We show that the VemP sequence has a low helical propensity in water and that the propensity is higher in more hydrophobic solvents. We propose that helix formation within the ribosome is driven by the tunnel environment and that a portion of VemP acts as an anchor. This anchor might slow down VemP progression through the tunnel enabling the α-helix formation, which causes the elongation arrest.
Kunkel John、Grubm¨1ller Helmut、Vaiana Sara M.、Nagy Gabor、Kol¨¢? Michal H.、Bock Lars V.
Department of Physics and Center for Biological Physics, Arizona State UniversityMax Planck Institute for Biophysical ChemistryDepartment of Physics and Center for Biological Physics, Arizona State UniversityMax Planck Institute for Biophysical ChemistryMax Planck Institute for Biophysical Chemistry||University of Chemistry and TechnologyMax Planck Institute for Biophysical Chemistry
生物物理学分子生物学生物化学
Kunkel John,Grubm¨1ller Helmut,Vaiana Sara M.,Nagy Gabor,Kol¨¢? Michal H.,Bock Lars V..Folding of VemP into translation-arresting secondary structure is driven by the ribosome exit tunnel[EB/OL].(2025-03-28)[2025-05-23].https://www.biorxiv.org/content/10.1101/2021.04.15.440051.点此复制
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