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The Proteasome Distinguishes between Heterotypic and Homotypic Lysine-11-Linked Polyubiquitin Chains.

Cell reports | 2015

Proteasome-mediated degradation occurs with proteins principally modified with lysine-48 polyubiquitin chains. Whether the proteasome also can bind atypical ubiquitin chains, including those linked by lysine-11, has not been well established. This is critically important, as lysine-11 polyubiquitination has been implicated in both proteasome-mediated degradation and non-degradative outcomes. Here we demonstrate that pure homotypic lysine-11-linked chains do not bind strongly to the mammalian proteasome. By contrast, heterotypic polyubiquitin chains, containing lysine-11 and lysine-48 linkages, not only bind to the proteasome but also stimulate the proteasomal degradation of the cell-cycle regulator cyclin B1. Thus, while heterotypic lysine-11-linked chains facilitate proteasomal degradation, homotypic lysine-11 linkages adopt conformations that prevent association with the proteasome. Our data demonstrate the capacity of the proteasome to bind ubiquitin chains of distinct topology, with implications for the recognition and diverse biological functions of mixed ubiquitin chains.

Pubmed ID: 26190103 RIS Download

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Associated grants

  • Agency: Medical Research Council, United Kingdom
    Id: G0802822
  • Agency: NIGMS NIH HHS, United States
    Id: R01 GM067945
  • Agency: NIGMS NIH HHS, United States
    Id: GM067945
  • Agency: Wellcome Trust, United Kingdom
    Id: 093966/Z/10/Z
  • Agency: Wellcome Trust, United Kingdom
    Id: 102770
  • Agency: Wellcome Trust, United Kingdom
    Id: 100140
  • Agency: Wellcome Trust, United Kingdom
    Id: 102770/Z/13/Z

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