2020
DOI: 10.1038/s41467-020-19504-3
|View full text |Cite
|
Sign up to set email alerts
|

Spatiotemporal dynamics of 53BP1 dimer recruitment to a DNA double strand break

Abstract: Tumor suppressor p53-binding protein 1 (53BP1) is a DNA repair protein essential for the detection, assessment, and resolution of DNA double strand breaks (DSBs). The presence of a DSB is signaled to 53BP1 via a local histone modification cascade that triggers the binding of 53BP1 dimers to chromatin flanking this type of lesion. While biochemical studies have established that 53BP1 exists as a dimer, it has never been shown in a living cell when or where 53BP1 dimerizes upon recruitment to a DSB site, or upon… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
1
1
1
1

Citation Types

2
21
0

Year Published

2021
2021
2024
2024

Publication Types

Select...
7
1

Relationship

2
6

Authors

Journals

citations
Cited by 29 publications
(23 citation statements)
references
References 53 publications
2
21
0
Order By: Relevance
“…Similar DNA break foci (as detected by 53BP1 and g-H2AX overlapping puncta), albeit fewer per neuron, were also found in the nuclei of DRG neurons as early as 10 min after a sciatic nerve crush injury (Figure 5A). Although the 53BP1 staining appears fuzzy in the nucleus, it localizes to foci in injured DRG neurons, which is the same as seen in other cell types (Harrigan et al, 2011;Lou et al, 2020;Shanbhag et al, 2019). The peak percentage of neurons with DSD foci occurred 30 min after the nerve injury, with a second but smaller increase at 24 h after the injury (Figure 5B).…”
Section: Sciatic Nerve Injury Induces Dna Breaks At the Atf3 Gene Locus In Drg Neuronssupporting
confidence: 65%
“…Similar DNA break foci (as detected by 53BP1 and g-H2AX overlapping puncta), albeit fewer per neuron, were also found in the nuclei of DRG neurons as early as 10 min after a sciatic nerve crush injury (Figure 5A). Although the 53BP1 staining appears fuzzy in the nucleus, it localizes to foci in injured DRG neurons, which is the same as seen in other cell types (Harrigan et al, 2011;Lou et al, 2020;Shanbhag et al, 2019). The peak percentage of neurons with DSD foci occurred 30 min after the nerve injury, with a second but smaller increase at 24 h after the injury (Figure 5B).…”
Section: Sciatic Nerve Injury Induces Dna Breaks At the Atf3 Gene Locus In Drg Neuronssupporting
confidence: 65%
“…To determine the stoichiometry of the NF-Y complex that was indirectly measured by consecutive FLIM-FRET detection of YA/YB/YC interaction in live cells, we next transfected HeLa cells with eGFP-YA, eGFP-YB or eGFP-YC and measured their respective oligomeric states via Number and Brightness (NB) analysis (Fig. 2 A–C) 30 , 31 . From comparison of the apparent brightness of eGFP-YB, eGFP-YC and eGFP-YA with the apparent brightness of our monomeric control eGFP we find each NF-Y subunit to be monomeric (Fig.…”
Section: Resultsmentioning
confidence: 99%
“…Accumulation and 53BP1 Recruitment to Damage Sites Induced by TMZ and Olaparib NHEJ is the main repair pathway of DSB (Pannunzio et al, 2018;Zhao et al, 2020). An intermediate step in the NHEJ pathway, is mediated by the formation of 53BP1 foci at DNA damage sites (Sanz-Garcia et al, 2012), which requires the accumulation of H4K20me2 (Jacquet et al, 2016;Guo et al, 2018;Lou et al, 2020). Therefore, we studied the effect of VRK1 depletion on the accumulation of H4K20me2, and the formation 53BP1 foci induced by TMZ and olaparib.…”
Section: Vrk1 Depletion Impairs H4k20me2mentioning
confidence: 99%