Xpo7 negatively regulates Hedgehog signaling by exporting Gli2 from the nucleus.

Cell Signal

Laboratory of Molecular and Cellular Signaling, Centre of New Technologies, University of Warsaw, Banacha 2c, 02-097 Warsaw, Poland. Electronic address:

Published: April 2021

AI Article Synopsis

  • Dynamic bidirectional transport between the nucleus and cytoplasm is essential for regulating transcription factors, particularly the Hedgehog (Hh) pathway, which relies on a balance of Gli protein forms.
  • Xpo7 is identified as a key nuclear export receptor that prevents Gli2 accumulation in the nucleus, influencing Hh signaling outcomes.
  • The interaction between Xpo7 and Gli2, modulated by the negative regulator SuFu, enhances understanding of Gli protein shuttling and transcription regulation.

Article Abstract

Dynamic bidirectional transport between the nucleus and the cytoplasm is critical for the regulation of many transcription factors, whose levels inside the nucleus must be tightly controlled. Efficient shuttling across the nuclear membrane is especially crucial with regard to the Hedgehog (Hh) pathway, where the transcriptional signal depends on the fine balance between the amounts of Gli protein activator and repressor forms in the nucleus. The nuclear export machinery prevents the unchecked nuclear accumulation of Gli proteins, but the mechanistic insight into this process is limited. We show that the atypical exportin Xpo7 functions as a major nuclear export receptor that actively excludes Gli2 from the nucleus and controls the outcome of Hh signaling. We show that Xpo7 interacts with several domains of Gli2 and that this interaction is modulated by SuFu, a key negative regulator of Hh signaling. Our data pave the way for a more complete understanding of the nuclear shuttling of Gli proteins and the regulation of their transcriptional activity.

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Source
http://dx.doi.org/10.1016/j.cellsig.2020.109907DOI Listing

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