NIH Resource for Macromolecular Modeling & Visualization University of Illinois at Urbana-Champaign

• Home
• Research
  • Driving Projects
  • Collaborations
  • Highlights
  • Viruses
  • Symbiont Bacteria
  • Molecular Motors
  • Neurons and Synapses
  • Bioenergetic Membranes
  • Nanosensors
  • Ribosome
  • Mechanosensing
  • Protein Folding
  • Integrative Modeling
  • More Topics
• Publications
  • Papers
  • Highly Cited
  • Representative
  • Covers
• Software
  • NAMD
    • Download
    • User's Guide
    • Mailing List
  • VMD
    • Download
    • Plugins
    • User's Guide
    • Mailing List
  • GPU Computing
  • Cloud Computing
  • Lattice Microbes
  • Atomic Resolution
    Brownian Dynamics
    
  • MDFF
  • QwikMD
  • VND (Neuronal)
  • Other
• Instruction
  • Training
  • Workshops
  • Seminars
  • Tutorials
  • Case Studies
  • Multimedia Lectures
  • Brochures
  • Classes
• News
• Galleries
  • Images
  • Movies
  • Posters
  • Brochures
  • Photos
• Facilities
  • Computational
  • Visitor
• About Us
  • Center Members
  • Mission
  • Brochures
  • Contact Us
  • Acknowledge Us

• Home

• Overview

• Publications

• Cover Pages

• Brochures

• Reports

• RSS Feed 

• Research

• Software

• Outreach

 

TCB
Publications

 

TCB Publications - Abstract

Shanmugapriya Sothiselvam, Bo Liu, Wei Han, Dorota Klepacki, Gemma C. Atkinson, Age Brauer, Maido Remm, Tanel Tenson, Klaus Schulten, Nora Vázquez-Laslop, and Alexander S. Mankin. Macrolide antibiotics allosterically predispose the ribosome for translation arrest. Proceedings of the National Academy of Sciences, USA, 111:9804-9809, 2014. (PMC: PMC4103360)

Programmed translation arrest directed by nascent peptides and small cofactors controls expression of important bacterial and eukaryotic genes. Inducible antibiotic resistance genes, activated by binding of macrolide molecules to the ribosome, are the most medically-relevant bacterial genes regulated by such mechanism. Previous studies suggested that specific interactions between the nascent peptide and the drug molecule juxtaposed in the ribosomal exit tunnel play a key role in the mechanism of translation arrest. However, here we show that macrolides can arrest translation of a truncated regulatory peptide ErmDL when the nascent chain is composed of only three amino acids and is thus too short to be juxtaposed with the antibiotic. Biochemical probing and all- atom molecular dynamics simulation of drug-free and erythromycin-bound ribosomes showed that binding of antibiotic in the tunnel allosterically alters the properties of the catalytic center, thereby predisposing the ribosome for arrest during translation of specific amino acid sequences. Our findings provide a principally new view on the role of small cofactors in the mechanism of programmed translation arrest and reveal an allosteric link between the exit tunnel and the catalytic center of the ribosome.

Download Full Text

The manuscripts available on our site are provided for your personal use only and may not be retransmitted or redistributed without written permissions from the paper's publisher and author. You may not upload any of this site's material to any public server, on-line service, network, or bulletin board without prior written permission from the publisher and author. You may not make copies for any commercial purpose. Reproduction or storage of materials retrieved from this web site is subject to the U.S. Copyright Act of 1976, Title 17 U.S.C.

Download full text: Journal, Request a Copy

Funded by a grant from
the National Institute of
General Medical Sciences
of the National Institutes
of Health

Beckman Institute for Advanced Science and Technology // National Institutes of Health // National Science Foundation // Physics, Computer Science, and Biophysics at University of Illinois at Urbana-Champaign

Contact Us // Material on this page is copyrighted; contact Webmaster for more information. // Document last modified on Mon Feb 14 10:51:08 2022 // 5454930 accesses since 20 Mar 2006 .