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Reference - PMID:23080121 - Mre11 ATLD17/18 mutation retains Tel1/ATM activity but blocks DNA double-strand break repair.

Reference summary

PubMed ID
PMID:23080121
Title
Mre11 ATLD17/18 mutation retains Tel1/ATM activity but blocks DNA double-strand break repair.
Authors
Limbo O, Moiani D, Kertokalio A, Wyman C, Tainer JA, Russell P
Citation
Nucleic Acids Res 2012 Dec;40(22):11435-49
Publication year
2012
Abstract
The Mre11 complex (Mre11-Rad50-Nbs1 or MRN) binds double-strand breaks where it interacts with CtIP/Ctp1/Sae2 and ATM/Tel1 to preserve genome stability through its functions in homology-directed repair, checkpoint signaling and telomere maintenance. Here, we combine biochemical, structural and in vivo functional studies to uncover key properties of Mre11-W243R, a mutation identified in two pediatric cancer patients with enhanced ataxia telangiectasia-like disorder. Purified human Mre11-W243R retains nuclease and DNA binding activities in vitro. X-ray crystallography of Pyrococcus furiosus Mre11 indicates that an analogous mutation leaves the overall Mre11 three-dimensional structure and nuclease sites intact but disorders surface loops expected to regulate DNA and Rad50 interactions. The equivalent W248R allele in fission yeast allows Mre11 to form an MRN complex that efficiently binds double-strand breaks, activates Tel1/ATM and maintains telomeres; yet, it causes hypersensitivity to ionizing radiation and collapsed replication forks, increased Rad52 foci, defective Chk1 signaling and meiotic failure. W248R differs from other ataxia telangiectasia-like disorder analog alleles by the reduced stability of its interaction with Rad50 in cell lysates. Collective results suggest a separation-of-function mutation that disturbs interactions amongst the MRN subunits and Ctp1 required for DNA end processing in vivo but maintains interactions sufficient for Tel1/ATM checkpoint and telomere maintenance functions.

Annotation

GO biological process

GO:0000729 - DNA double-strand break processing

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GO cellular component

GO:0035861 - site of double-strand break

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GO molecular function

GO:0005515 - protein binding

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Single locus phenotype

FYPO:0000121 - abnormal sporulation

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FYPO:0000913 - abnormal sporulation resulting in formation of ascus containing non-uniform spores

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FYPO:0000705 - abolished protein-protein interaction

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FYPO:0001407 - decreased cell population growth on glucose carbon source

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FYPO:0000218 - decreased Mre11 complex assembly

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FYPO:0001324 - decreased protein level during vegetative growth

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FYPO:0002474 - decreased protein localization to double-strand break site

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FYPO:0002470 - decreased protein phosphorylation during cellular response to ionizing radiation

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FYPO:0001645 - decreased protein-protein interaction

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FYPO:0000581 - decreased spore germination frequency

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FYPO:0000972 - increased number of Rad52 foci during vegetative growth

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FYPO:0002475 - increased protein localization to double-strand break site

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FYPO:0002169 - normal growth during cellular response to gamma radiation

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FYPO:0000969 - normal growth during cellular response to UV

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FYPO:0001690 - normal growth on camptothecin

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FYPO:0001164 - normal growth on glucose carbon source

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FYPO:0000963 - normal growth on hydroxyurea

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FYPO:0000703 - normal protein-protein interaction

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FYPO:0000085 - sensitive to camptothecin

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FYPO:0000266 - sensitive to DNA damaging agents

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FYPO:0000088 - sensitive to hydroxyurea

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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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FYPO:0000268 - sensitive to UV during vegetative growth

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FYPO:0001492 - viable elongated vegetative cell

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