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Mechanism of signal sequence handover from NAC to SRP on ribosomes during ER-protein targeting

Science, ISSN: 1095-9203, Vol: 375, Issue: 6583, Page: 839-844
2022
  • 44
    Citations
  • 0
    Usage
  • 103
    Captures
  • 3
    Mentions
  • 2
    Social Media
Metric Options:   Counts1 Year3 Year

Metrics Details

  • Citations
    44
  • Captures
    103
  • Mentions
    3
    • News Mentions
      2
      • 2
    • References
      1
      • 1
  • Social Media
    2
    • Shares, Likes & Comments
      2
      • Facebook
        2

Most Recent News

Exchange at Ribosomal Exit Targets Newborn Proteins to the ER

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Article Description

The nascent polypeptide–associated complex (NAC) interacts with newly synthesized proteins at the ribosomal tunnel exit and competes with the signal recognition particle (SRP) to prevent mistargeting of cytosolic and mitochondrial polypeptides to the endoplasmic reticulum (ER). How NAC antagonizes SRP and how this is overcome by ER targeting signals are unknown. Here, we found that NAC uses two domains with opposing effects to control SRP access. The core globular domain prevented SRP from binding to signal-less ribosomes, whereas a flexibly attached domain transiently captured SRP to permit scanning of nascent chains. The emergence of an ER-targeting signal destabilized NAC’s globular domain and facilitated SRP access to the nascent chain. These findings elucidate how NAC hands over the signal sequence to SRP and imparts specificity of protein localization.

Bibliographic Details

Jomaa, Ahmad; Gamerdinger, Martin; Hsieh, Hao-Hsuan; Wallisch, Annalena; Chandrasekaran, Viswanathan; Ulusoy, Zeynel; Scaiola, Alain; Hegde, Ramanujan S; Shan, Shu-Ou; Ban, Nenad; Deuerling, Elke

American Association for the Advancement of Science (AAAS)

Multidisciplinary

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