Phosphorylation-dependent assembly of DNA damage response systems and the central roles of TOPBP1

The cellular response to DNA damage (DDR) that causes replication collapse and/or DNA double strand breaks, is characterised by a massive change in the post-translational modifications (PTM) of hundreds of proteins involved in the detection and repair of DNA damage, and the communication of the stat...

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Published in:DNA repair 2021-12, Vol.108, p.103232-103232, Article 103232
Main Authors: Day, Matthew, Oliver, Antony W., Pearl, Laurence H.
Format: Article
Language:English
Subjects:
BRCT domains
Carrier Proteins - metabolism
Cell Cycle Proteins - metabolism
Checkpoints
DNA Damage
DNA damage response
DNA Repair
DNA-Binding Proteins - metabolism
Nuclear Proteins - metabolism
Phosphopeptide binding
Phosphorylation
Protein-protein interactions
Specificity
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container_title DNA repair
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creator Day, Matthew
Oliver, Antony W.
Pearl, Laurence H.
description The cellular response to DNA damage (DDR) that causes replication collapse and/or DNA double strand breaks, is characterised by a massive change in the post-translational modifications (PTM) of hundreds of proteins involved in the detection and repair of DNA damage, and the communication of the state of damage to the cellular systems that regulate replication and cell division. A substantial proportion of these PTMs involve targeted phosphorylation, which among other effects, promotes the formation of multiprotein complexes through the specific binding of phosphorylated motifs on one protein, by specialised domains on other proteins. Understanding the nature of these phosphorylation mediated interactions allows definition of the pathways and networks that coordinate the DDR, and helps identify new targets for therapeutic intervention that may be of benefit in the treatment of cancer, where DDR plays a key role. In this review we summarise the present understanding of how phosphorylated motifs are recognised by BRCT domains, which occur in many DDR proteins. We particularly focus on TOPBP1 – a multi-BRCT domain scaffold protein with essential roles in replication and the repair and signalling of DNA damage.
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subjects BRCT domains
Carrier Proteins - metabolism
Cell Cycle Proteins - metabolism
Checkpoints
DNA Damage
DNA damage response
DNA Repair
DNA-Binding Proteins - metabolism
Nuclear Proteins - metabolism
Phosphopeptide binding
Phosphorylation
Protein-protein interactions
Specificity
title Phosphorylation-dependent assembly of DNA damage response systems and the central roles of TOPBP1
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