Structure of the Tuberous Sclerosis Complex 2 (TSC2) N Terminus Provides Insight into Complex Assembly and Tuberous Sclerosis Pathogenesis*

  1. Daniel Kümmel1
  1. From the Structural Biology Section, FB5 Biology/Chemistry, University of Osnabrück, 49076 Osnabrück, Germany,
  2. §Macromolecular Crystallography (BESSY-MX), Helmholtz-Zentrum Berlin für Materialien und Energie, 12489 Berlin, Germany, and
  3. Institute of Molecular Tumor Biology, Medical Faculty of the WWU Münster, 48149 Münster Germany
  1. 1 To whom correspondence should be addressed: FB5 Biology/Chemistry, University of Osnabrück, Barbarastr. 13, 49076 Osnabrück, Germany. Tel.: 49-541-9693423; Fax: 40-541-9692884; E-mail: daniel.kuemmel{at}uos.de.

Abstract

Tuberous sclerosis complex (TSC) is caused by mutations in the TSC1 and TSC2 tumor suppressor genes. The gene products hamartin and tuberin form the TSC complex that acts as GTPase-activating protein for Rheb and negatively regulates the mammalian target of rapamycin complex 1 (mTORC1). Tuberin contains a RapGAP homology domain responsible for inactivation of Rheb, but functions of other protein domains remain elusive. Here we show that the TSC2 N terminus interacts with the TSC1 C terminus to mediate complex formation. The structure of the TSC2 N-terminal domain from Chaetomium thermophilum and a homology model of the human tuberin N terminus are presented. We characterize the molecular requirements for TSC1-TSC2 interactions and analyze pathological point mutations in tuberin. Many mutations are structural and produce improperly folded protein, explaining their effect in pathology, but we identify one point mutant that abrogates complex formation without affecting protein structure. We provide the first structural information on TSC2/tuberin with novel insight into the molecular function.

Footnotes

  • * This work was supported by Deutsche Forschungsgemeinschaft Grants KU 2531/2-1 and SFB 944-P17 (to D. K.) and OE 531/2-1 (to A. O.). The authors declare that they have no conflicts of interest with the contents of this article.

  • Graphic This article contains supplemental Fig. S1.

  • Received April 13, 2016.
  • Revision received July 27, 2016.
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  1. First Published on August 4, 2016 doi: 10.1074/jbc.M116.732446 The Journal of Biological Chemistry 291, 20008-20020.
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