Disorder and residual helicity alter p53-Mdm2

Abstract

Levels of residual structure in disordered interaction domains determine in vitro binding affinities, but whether they exert similar roles in cells is not known. Here, we show that increasing residual p53 helicity results in stronger Mdm2 binding, altered p53 dynamics, impaired target gene expression and failure to induce cell cycle arrest upon DNA damage. These results establish that residual structure is an important determinant of signaling fidelity in cells.

Details

Title

Disorder and residual helicity alter p53-Mdm2 binding affinity and signaling in cells

Author

Borcherds, Wade; Theillet, François-xavier; Katzer, Andrea; Finzel, Ana; Mishall, Katie M; Powell, Anne T; Wu, Hongwei; Manieri, Wanda; Dieterich, Christoph; Selenko, Philipp; Loewer, Alexander; Daughdrill, Gary W

Pages

1000-2

Publication year

2014

Publication date

Dec 2014

Publisher

Nature Publishing Group

ISSN

15524450

e-ISSN

15524469

Source type

Scholarly Journal

Language of publication

English

DOI

https://doi.org/10.1038/nchembio.1668

ProQuest document ID

1647096271

Disorder and residual helicity alter p53-Mdm2 binding affinity and signaling in cells

Content area

Abstract

Details

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