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. 2021 Mar 18;81(6):1231-1245.e8.
doi: 10.1016/j.molcel.2020.12.049. Epub 2021 Jan 26.

TopBP1 assembles nuclear condensates to switch on ATR signaling

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TopBP1 assembles nuclear condensates to switch on ATR signaling

Camilla Frattini et al. Mol Cell. .
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Abstract

ATR checkpoint signaling is crucial for cellular responses to DNA replication impediments. Using an optogenetic platform, we show that TopBP1, the main activator of ATR, self-assembles extensively to yield micrometer-sized condensates. These opto-TopBP1 condensates are functional entities organized in tightly packed clusters of spherical nano-particles. TopBP1 condensates are reversible, occasionally fuse, and co-localize with TopBP1 partner proteins. We provide evidence that TopBP1 condensation is a molecular switch that amplifies ATR activity to phosphorylate checkpoint kinase 1 (Chk1) and slow down replication forks. Single amino acid substitutions of key residues in the intrinsically disordered ATR activation domain disrupt TopBP1 condensation and consequently ATR/Chk1 signaling. In physiologic salt concentration and pH, purified TopBP1 undergoes liquid-liquid phase separation in vitro. We propose that the actuation mechanism of ATR signaling is the assembly of TopBP1 condensates driven by highly regulated multivalent and cooperative interactions.

Keywords: ATR; DNA damage response; DNA replication; S phase checkpoint; TopBP1; biomolecular condensates; liquid phase separation; optogenetics; proximity-labeling proteomics; signal transduction.

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Conflict of interest statement

Declaration of interests The authors declare no competing interests.

Comment in

  • TopBP1 comes into focus.
    Dunphy WG. Dunphy WG. Mol Cell. 2021 Mar 18;81(6):1126-1127. doi: 10.1016/j.molcel.2021.02.027. Mol Cell. 2021. PMID: 33740471

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