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Details

Autor(en) / Beteiligte
Titel
Folding Mechanism of an Ankyrin Repeat Protein: Scaffold and Active Site Formation of Human CDK Inhibitor p19 INK4d
Ist Teil von
  • Journal of molecular biology, 2007, Vol.373 (1), p.219-231
Ort / Verlag
Elsevier Ltd
Erscheinungsjahr
2007
Link zum Volltext
Quelle
Elsevier ScienceDirect Journals Complete
Beschreibungen/Notizen
  • The p19 INK4d protein consists of five ankyrin repeats (ANK) and controls the human cell cycle by inhibiting the cyclin D-dependent kinases (CDK) 4 and 6. We investigated the folding of p19 INK4d by urea-induced unfolding transitions, kinetic analyses of unfolding and refolding, including double-mixing experiments and a special assay for folding intermediates. Folding is a sequential two-step reaction via a hyperfluorescent on-pathway intermediate. This intermediate is present under all conditions, during unfolding, refolding and at equilibrium. The folding mechanism was confirmed by a quantitative global fit of a consistent set of equilibrium and kinetic data revealing the thermodynamics and intrinsic folding rates of the different states. Surprisingly, the N ↔ I transition is much faster compared to the I ↔ U transition. The urea-dependence of the intrinsic folding rates causes population of the intermediate at equilibrium close to the transition midpoint. NMR detected hydrogen/deuterium exchange and the analysis of truncated variants showed that the C-terminal repeats ANK3-5 are already folded in the on-pathway intermediate, whereas the N-terminal repeats 1 and 2 are not folded. We suggest that during refolding, repeats ANK3–ANK5 first form the scaffold for the subsequent assembly of repeats ANK1 and ANK2. The binding function of p19 INK4d resides in the latter repeats. We propose that the graded stability and the facile unfolding of repeats 1 and 2 is a prerequisite for the down-regulation of the inhibitory activity of p19 INK4d during the cell-cycle.
Sprache
Englisch
Identifikatoren
ISSN: 0022-2836
eISSN: 1089-8638
DOI: 10.1016/j.jmb.2007.07.063
Titel-ID: cdi_elsevier_sciencedirect_doi_10_1016_j_jmb_2007_07_063

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