Site-specific acetylation mark on an essential chromatin-remodeling complex promotes resistance to replication stress

Charles, Georgette M.; Chen, Changbin; Shih, Susan C.; Collins, Sean R.; Beltrao, Pedro; Zhang, Xin; Sharma, Tanu; Tan, Song; Burlingame, Alma L.; Krogan, Nevan J.; Madhani, Hiten D.; Narlikar, Geeta J.

doi:10.1073/pnas.1019735108

Site-specific acetylation mark on an essential chromatin-remodeling complex promotes resistance to replication stress

METADATA ONLY

Author / Producer

Charles, Georgette M.

Chen, Changbin

Shih, Susan C.

Date

2011-06-28

Publication Type

Journal Article

ETH Bibliography

no

METADATA ONLY

Abstract

Recent work has identified several posttranslational modifications (PTMs) on chromatin-remodeling complexes. Compared with our understanding of histone PTMs, significantly less is known about the functions of PTMs on remodeling complexes, because identification of their specific roles often is hindered by the presence of redundant pathways. Remodels the Structure of Chromatin (RSC) is an essential, multifunctional ATP-dependent chromatin-remodeling enzyme of Saccharomyces cerevisiae that preferentially binds acetylated nucleosomes. RSC is itself acetylated by Gcn5 on lysine 25 (K25) of its Rsc4 subunit, adjacent to two tandem bromodomains. It has been shown that an intramolecular interaction between the acetylation mark and the proximal bromodomain inhibits binding of the second bromodomain to acetylated histone H3 tails. We report here that acetylation does not significantly alter the catalytic activity of RSC or its ability to recognize histone H3-acetylated nucleosomes preferentially in vitro. However, we find that Rsc4 acetylation is crucial for resistance to DNA damage in vivo. Epistatic miniarray profiling of the rsc4-K25R mutant reveals an interaction with mutants in the INO80 complex, a mediator of DNA damage and replication stress tolerance. In the absence of a core INO80 subunit, rsc4-K25R mutants display sensitivity to hydroxyurea and delayed S-phase progression under DNA damage. Thus, Rsc4 helps promote resistance to replication stress, and its single acetylation mark regulates this function. These studies offer an example of acetylation of a chromatin-remodeling enzyme controlling a biological output of the system rather than regulating its core enzymatic properties.

Permanent link

http://hdl.handle.net/20.500.11850/531908

Publication status

published

External links

https://doi.org/10.1073/pnas.1019735108 north_east

Journal / series

Proceedings of the National Academy of Sciences of the United States of America north_east

Volume

108 (26)

Pages / Article No.

10620 - 10625

Publisher

National Academy of Sciences

Organisational unit

09758 - Beltrao, Pedro / Beltrao, Pedro

More

Show all metadata

Site-specific acetylation mark on an essential chromatin-remodeling complex promotes resistance to replication stress

Author / Producer

Date

Publication Type

ETH Bibliography

Citations

Altmetric

Data

Rights / License

Abstract

Permanent link

Publication status

External links

Editor

Book title

Journal / series

Volume

Pages / Article No.

Publisher

Event

Edition / version

Methods

Software

Geographic location

Date collected

Date created

Subject

Organisational unit

Notes

Funding

Related publications and datasets

More