NDLI: The complexity of phosphorylated H2AX foci formation and DNA repair assembly at DNA double-strand breaks

Please wait, while we are loading the content...

The complexity of phosphorylated H2AX foci formation and DNA repair assembly at DNA double-strand breaks

Content Provider	Scilit
Author	Nakamura, Asako J. Rao, V. Ashutosh Pommier, Yves Bonner, William M.
Copyright Year	2010
Description	The maintenance of genome stability requires efficient DNA double-stranded break (DSB) repair mediated by the phosphorylation of multiple histone H2AX molecules near the break sites. The phosphorylated H2AX (γH2AX) molecules form foci covering many megabases of chromatin. the formation of γ-H2AX foci is critical for efficient DNA damage response (DDR) and for the maintenance of genome stability, however, the mechanisms of protein organization in foci is largely unknown. To investigate the nature of γH2AX foci formation, we analyzed the distribution of γH2AX and other DDR proteins at DSB sites using a variety of techniques to visualize, expand and partially disrupt chromatin. We report here that γH2AX foci change composition during the cell cycle, with proteins 53BP1, NBS1 and MRE11 dissociating from foci in G2 and mitosis to return at the beginning of the following G1. In contrast, MDC1 remained colocalized with γ-H2AX during mitosis. In addition, while γH2AX was found to span large domains flanking DSB sites, 53BP1 and NBS1 were more localized and MDC1 colocalized in doublets in foci. H2AX and MDC1 were found to be involved in chromatin relaxation after DSB formation. Our data demonstrates that the DSB repair focus is a heterogeneous and dynamic structure containing internal complexity.
Related Links	https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3086803/pdf
Ending Page	397
Page Count	9
Starting Page	389
ISSN	15384101
e-ISSN	15514005
DOI	10.4161/cc.9.2.10475
Journal	Cell Cycle
Issue Number	2
Volume Number	9
Language	English
Publisher	Informa UK Limited
Publisher Date	2010-01-15
Access Restriction	Open
Subject Keyword	Journal: Cell Cycle Biochemistry and Molecular Biology Dna Double Strand Breaks Phosphorylated H2ax Mdc1 53bp1 Nbs1
Content Type	Text
Resource Type	Article
Subject	Cell Biology Developmental Biology Medicine Molecular Biology

Sl.	Authority	Responsibilities	Communication Details
1	Ministry of Education (GoI), Department of Higher Education	Sanctioning Authority	https://www.education.gov.in/ict-initiatives
2	Indian Institute of Technology Kharagpur	Host Institute of the Project: The host institute of the project is responsible for providing infrastructure support and hosting the project	https://www.iitkgp.ac.in
3	National Digital Library of India Office, Indian Institute of Technology Kharagpur	The administrative and infrastructural headquarters of the project	Dr. B. Sutradhar bsutra@ndl.gov.in
4	Project PI / Joint PI	Principal Investigator and Joint Principal Investigators of the project	Dr. B. Sutradhar bsutra@ndl.gov.in Prof. Saswat Chakrabarti will be added soon
5	Website/Portal (Helpdesk)	Queries regarding NDLI and its services	support@ndl.gov.in
6	Contents and Copyright Issues	Queries related to content curation and copyright issues	content@ndl.gov.in
7	National Digital Library of India Club (NDLI Club)	Queries related to NDLI Club formation, support, user awareness program, seminar/symposium, collaboration, social media, promotion, and outreach	clubsupport@ndl.gov.in
8	Digital Preservation Centre (DPC)	Assistance with digitizing and archiving copyright-free printed books	dpc@ndl.gov.in
9	IDR Setup or Support	Queries related to establishment and support of Institutional Digital Repository (IDR) and IDR workshops	idr@ndl.gov.in

The complexity of phosphorylated H2AX foci formation and DNA repair assembly at DNA double-strand breaks

Phosphorylation-regulated binding of Ctp1 to Nbs1 is critical for repair of DNA double-strand breaks.

DNA double strand breaks: not all foci are created equal.

Cell Cycle-Regulated Centers of DNA Double-Strand Break Repair

Recruitment of proteins to DNA double-strand breaks: MDC1 directly recruits RAP80

Loop extrusion as a mechanism for DNA Double-Strand Breaks repair foci formation

MDC1 Directly Binds Phosphorylated Histone H2AX to Regulate Cellular Responses to DNA Double-Strand Breaks

Fanconi Anemia Is Characterized by Delayed Repair Kinetics of DNA Double-Strand Breaks

Dynamics of Chromatin during the Repair of DNA Double-Strand Breaks

The complexity of phosphorylated H2AX foci formation and DNA repair assembly at DNA double-strand breaks

Similar Documents

The complexity of phosphorylated H2AX foci formation and DNA repair assembly at DNA double-strand breaks

Phosphorylation-regulated binding of Ctp1 to Nbs1 is critical for repair of DNA double-strand breaks.

DNA double strand breaks: not all foci are created equal.

Cell Cycle-Regulated Centers of DNA Double-Strand Break Repair

Recruitment of proteins to DNA double-strand breaks: MDC1 directly recruits RAP80

Loop extrusion as a mechanism for DNA Double-Strand Breaks repair foci formation

MDC1 Directly Binds Phosphorylated Histone H2AX to Regulate Cellular Responses to DNA Double-Strand Breaks

Fanconi Anemia Is Characterized by Delayed Repair Kinetics of DNA Double-Strand Breaks

Dynamics of Chromatin during the Repair of DNA Double-Strand Breaks

The complexity of phosphorylated H2AX foci formation and DNA repair assembly at DNA double-strand breaks