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Reference - PMID:15964794 - ATM activation and its recruitment to damaged DNA require binding to the C terminus of Nbs1.

Reference summary

PubMed ID
PMID:15964794
Title
ATM activation and its recruitment to damaged DNA require binding to the C terminus of Nbs1.
Authors
You Z, Chahwan C, Bailis J, Hunter T, Russell P
Citation
Mol Cell Biol 2005 Jul;25(13):5363-79
Publication year
2005
Abstract
ATM has a central role in controlling the cellular responses to DNA damage. It and other phosphoinositide 3-kinase-related kinases (PIKKs) have giant helical HEAT repeat domains in their amino-terminal regions. The functions of these domains in PIKKs are not well understood. ATM activation in response to DNA damage appears to be regulated by the Mre11-Rad50-Nbs1 (MRN) complex, although the exact functional relationship between the MRN complex and ATM is uncertain. Here we show that two pairs of HEAT repeats in fission yeast ATM (Tel1) interact with an FXF/Y motif at the C terminus of Nbs1. This interaction resembles nucleoporin FXFG motif binding to HEAT repeats in importin-beta. Budding yeast Nbs1 (Xrs2) appears to have two FXF/Y motifs that interact with Tel1 (ATM). In Xenopus egg extracts, the C terminus of Nbs1 recruits ATM to damaged DNA, where it is subsequently autophosphorylated. This interaction is essential for ATM activation. A C-terminal 147-amino-acid fragment of Nbs1 that has the Mre11- and ATM-binding domains can restore ATM activation in an Nbs1-depleted extract. We conclude that an interaction between specific HEAT repeats in ATM and the C-terminal FXF/Y domain of Nbs1 is essential for ATM activation. We propose that conformational changes in the MRN complex that occur upon binding to damaged DNA are transmitted through the FXF/Y-HEAT interface to activate ATM. This interaction also retains active ATM at sites of DNA damage.

Annotation

Multi-locus phenotype

FYPO:0002472 - abolished histone H2A phosphorylation during cellular response to ionizing radiation

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FYPO:0004869 - decreased number of Crb2 foci during cellular response to ionizing radiation

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FYPO:0001355 - decreased vegetative cell population growth

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Single locus phenotype

FYPO:0000705 - abolished protein-protein interaction

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FYPO:0004229 - normal growth during cellular response to ionizing radiation

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FYPO:0000957 - normal growth on methyl methanesulfonate

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FYPO:0000703 - normal protein-protein interaction

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FYPO:0000267 - sensitive to ionizing radiation during vegetative growth

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FYPO:0000089 - sensitive to methyl methanesulfonate

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