The Molecular Basis for Phosphodependent Substrate Targeting and Regulation of Plks by the Polo-box Domain

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2003 Oct 9

PMID 14532005

Citations 386

Authors

Andrew E H Elia

Peter Rellos

Lesley F Haire

Jerry W Chao

Frank J Ivins

Katja Hoepker

Duaa Mohammad

Lewis C Cantley

Stephen J Smerdon

Michael B Yaffe

Affiliations

Soon will be listed here.

Abstract

Polo-like kinases (Plks) perform crucial functions in cell-cycle progression and multiple stages of mitosis. Plks are characterized by a C-terminal noncatalytic region containing two tandem Polo boxes, termed the Polo-box domain (PBD), which has recently been implicated in phosphodependent substrate targeting. We show that the PBDs of human, Xenopus, and yeast Plks all recognize similar phosphoserine/threonine-containing motifs. The 1.9 A X-ray structure of a human Plk1 PBD-phosphopeptide complex shows that the Polo boxes each comprise beta6alpha structures that associate to form a 12-stranded beta sandwich domain. The phosphopeptide binds along a conserved, positively charged cleft located at the edge of the Polo-box interface. Mutations that specifically disrupt phosphodependent interactions abolish cell-cycle-dependent localization and provide compelling phenotypic evidence that PBD-phospholigand binding is necessary for proper mitotic progression. In addition, phosphopeptide binding to the PBD stimulates kinase activity in full-length Plk1, suggesting a conformational switching mechanism for Plk regulation and a dual functionality for the PBD.

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