nucleosome-binding protein HMGN2 modulates global genome repair

The HMGN family comprises nuclear proteins that bind to nucleosomes and alter the structure of chromatin. Here, we report that DT40 chicken cells lacking either HMGN2 or HMGN1a, or lacking both HMGN1a and HMGN2, are hypersensitive to killing by UV irradiation. Loss of both HMGN1a and HMGN2 or only H...

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Bibliographic Details
Published in:The FEBS journal 2009-11, Vol.276 (22), p.6646-6657
Main Authors: Subramanian, Mangalam, Gonzalez, Rhiannon W, Patil, Hemangi, Ueda, Takahiro, Lim, Jae-Hwan, Kraemer, Kenneth H, Bustin, Michael, Bergel, Michael
Format: Article
Language:English
Subjects:
Animals
apoptosis
Apoptosis - radiation effects
Biochemistry
Blotting, Southwestern
Blotting, Western
cell cycle
Cell Cycle - radiation effects
Cell Survival - radiation effects
Chickens
Chromatin
Chromatin - genetics
DNA Repair
Genome - genetics
Genomics
HMGN1 Protein - metabolism
HMGN2 Protein - genetics
HMGN2 Protein - metabolism
Mutation
Proteins
Ultraviolet Rays
UV irradiation
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Summary:The HMGN family comprises nuclear proteins that bind to nucleosomes and alter the structure of chromatin. Here, we report that DT40 chicken cells lacking either HMGN2 or HMGN1a, or lacking both HMGN1a and HMGN2, are hypersensitive to killing by UV irradiation. Loss of both HMGN1a and HMGN2 or only HMGN2 increases the extent of UV-induced Gâ‚‚-M checkpoint arrest and the rate of apoptosis. HMGN null mutant cells showed slower removal of UV-induced DNA lesions from native chromatin, but the nucleotide excision repair remained intact, as measured by host cell reactivation assays. These results identify HMGN2 as a component of the global genome repair subpathway of the nucleotide excision repair pathway, and may indicate that HMGN2 facilitates the ability of the DNA repair proteins to access and repair UV-induced DNA lesions in chromatin. Our finding that HMGNs play a role in global DNA repair expands the role of these proteins in the maintenance of genome integrity.
ISSN:1742-464X
1742-4658
DOI:10.1111/j.1742-4658.2009.07375.x