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Myosin-1C uses a novel phosphoinositide-dependent pathway for nuclear localization. | LitMetric

Myosin-1C uses a novel phosphoinositide-dependent pathway for nuclear localization.

EMBO Rep

Program in Cell and Molecular Biology, Institute of Biotechnology, University of Helsinki, Helsinki, Finland

Published: February 2018

AI Article Synopsis

  • - The study challenges the traditional view of how proteins enter the nucleus by demonstrating that Myosin-1C (Myo1C) relies on a diffusion-retention mechanism rather than the expected nuclear localization signals and transport factors.
  • - Myo1C is shown to continuously shuttle between the nucleus and cytoplasm, with its nuclear import being linked to its interaction with the endoplasmic reticulum and requiring phosphoinositide binding.
  • - This research suggests that membrane association and interaction with nuclear partners can drive the nuclear localization of soluble proteins, offering new insights into cellular protein sorting processes.

Article Abstract

Accurate control of macromolecule transport between nucleus and cytoplasm underlines several essential biological processes, including gene expression. According to the canonical model, nuclear import of soluble proteins is based on nuclear localization signals and transport factors. We challenge this view by showing that nuclear localization of the actin-dependent motor protein Myosin-1C (Myo1C) resembles the diffusion-retention mechanism utilized by inner nuclear membrane proteins. We show that Myo1C constantly shuttles in and out of the nucleus and that its nuclear localization does not require soluble factors, but is dependent on phosphoinositide binding. Nuclear import of Myo1C is preceded by its interaction with the endoplasmic reticulum, and phosphoinositide binding is specifically required for nuclear import, but not nuclear retention, of Myo1C. Our results therefore demonstrate, for the first time, that membrane association and binding to nuclear partners is sufficient to drive nuclear localization of also soluble proteins, opening new perspectives to evolution of cellular protein sorting mechanisms.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5797967PMC
http://dx.doi.org/10.15252/embr.201744296DOI Listing

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