Ubiquitin-dependent recruitment of the Bloom Syndrome helicase upon replication stress is required to suppress homologous recombination

Tikoo, Shweta ; Madhavan, Vinoth ; Hussain, Mansoor ; Miller, Edward S. ; Arora, Prateek ; Zlatanou, Anastasia ; Modi, Priyanka ; Townsend, Kelly ; Stewart, Grant S. ; Sengupta, Sagar (2013) Ubiquitin-dependent recruitment of the Bloom Syndrome helicase upon replication stress is required to suppress homologous recombination EMBO Journal, 32 (12). pp. 1778-1792. ISSN 0261-4189

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Official URL: http://emboj.embopress.org/content/32/12/1778.long

Related URL: http://dx.doi.org/10.1038/emboj.2013.117

Abstract

Limiting the levels of homologous recombination (HR) that occur at sites of DNA damage is a major role of BLM helicase. However, very little is known about the mechanisms dictating its relocalization to these sites. Here, we demonstrate that the ubiquitin/SUMO‐dependent DNA damage response (UbS‐DDR), controlled by the E3 ligases RNF8/RNF168, triggers BLM recruitment to sites of replication fork stalling via ubiquitylation in the N‐terminal region of BLM and subsequent BLM binding to the ubiquitin‐interacting motifs of RAP80. Furthermore, we show that this mechanism of BLM relocalization is essential for BLM's ability to suppress excessive/uncontrolled HR at stalled replication forks. Unexpectedly, we also uncovered a requirement for RNF8‐dependent ubiquitylation of BLM and PML for maintaining the integrity of PML‐associated nuclear bodies and as a consequence the localization of BLM to these structures. Lastly, we identified a novel role for RAP80 in preventing proteasomal degradation of BLM in unstressed cells. Taken together, these data highlight an important biochemical link between the UbS‐DDR and BLM‐dependent pathways involved in maintaining genome stability.

Item Type:Article
Source:Copyright of this article belongs to EMBO Press.
Keywords:RAP80; RNF8; RNF168; K63‐Linked Ubiquitylation; PML Nuclear Bodies
ID Code:111453
Deposited On:31 Jan 2018 09:36
Last Modified:31 Jan 2018 09:36

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