Article

  • The EMBO Journal (2004) 23, 3227 - 3236
  • doi:10.1038/sj.emboj.7600338

Published online: 29 July 2004

Exportin 7 defines a novel general nuclear export pathway

José-Manuel Mingot, Markus T Bohnsack, Ursula Jäkle and Dirk Görlich

  1. ZMBH, INF 282, Heidelberg, Germany

Correspondence to:

Dirk Görlich, ZMBH, Universität Heidelberg, Im Neuenheimer Feld 282, 69120 Heidelberg, Germany. Tel.: +49 6221 545884; Fax: +49 6221 545893; E-mail: dg@zmbh.uni-heidelberg.de

Received 23 January 2004; Accepted 29 June 2004


Most transport pathways between cell nucleus and cytoplasm are mediated by nuclear transport receptors of the importin beta family. These receptors are in continuous circulation between the two compartments and transfer cargo molecules from one side of the nuclear envelope to the other. RanBP16 is a family member from higher eukaryotes of so far unknown function. We now show that it exports p50RhoGAP from the nucleus and thereby confines this activity to the cytoplasm. It also accounts for nuclear exclusion of 14-3-3sigma, which in turn is known to anchor, for example, cyclin-dependent kinases in the cytoplasm. Our data further suggest that RanBP16 exports several additional cargoes. It thus appears to be a nuclear export mediator with broad substrate specificity and we will therefore refer to it as exportin 7 (Exp7). Finally, we demonstrate that Exp7-dependent nuclear export signals differ fundamentally from the leucine-rich, CRM1-dependent ones: First, they are not just short linear sequences, but instead include folded motifs. Second, basic residues are critical for Exp7 recruitment.

  • Keywords:

    • 14-3-3,
    • nuclear pore complex,
    • p50RhoGAP,
    • RanGTPase,
    • Xpo7
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