Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication

Dongyi Xu; Parameswary Muniandy; Elisabetta Leo; Jinhu Yin; Saravanabhavan Thangavel; Xi Shen; Miki Ii; Keli Agama; Rong Guo; David Fox; Amom Ruhikanta Meetei; Lauren Wilson; Huy Nguyen; Nan Ping Weng; Steven J. Brill; Lei Li; Alessandro Vindigni; Yves Pommier; Michael Seidman; Weidong Wang

doi:10.1038/emboj.2010.186

Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication

Dongyi Xu, Parameswary Muniandy, Elisabetta Leo, Jinhu Yin, Saravanabhavan Thangavel, Xi Shen, Miki Ii, Keli Agama, Rong Guo, David Fox, Amom Ruhikanta Meetei, Lauren Wilson, Huy Nguyen, Nan Ping Weng, Steven J. Brill, Lei Li, Alessandro Vindigni, Yves Pommier, Michael Seidman, Weidong Wang

Experimental Radiation Oncology

Research output: Contribution to journal › Article › peer-review

79 Scopus citations

Abstract

BLM, the helicase defective in Bloom syndrome, is part of a multiprotein complex that protects genome stability. Here, we show that Rif1 is a novel component of the BLM complex and works with BLM to promote recovery of stalled replication forks. First, Rif1 physically interacts with the BLM complex through a conserved C-terminal domain, and the stability of Rif1 depends on the presence of the BLM complex. Second, Rif1 and BLM are recruited with similar kinetics to stalled replication forks, and the Rif1 recruitment is delayed in BLM-deficient cells. Third, genetic analyses in vertebrate DT40 cells suggest that BLM and Rif1 work in a common pathway to resist replication stress and promote recovery of stalled forks. Importantly, vertebrate Rif1 contains a DNA-binding domain that resembles the Î ±CTD domain of bacterial RNA polymerase Î ±; and this domain preferentially binds fork and Holliday junction (HJ) DNA in vitro and is required for Rif1 to resist replication stress in vivo. Our data suggest that Rif1 provides a new DNA-binding interface for the BLM complex to restart stalled replication forks.

Original language	English (US)
Pages (from-to)	3140-3155
Number of pages	16
Journal	EMBO Journal
Volume	29
Issue number	18
DOIs	https://doi.org/10.1038/emboj.2010.186
State	Published - Sep 2010

Keywords

BLM
Bloom syndrome
RMI
Rif1
replication

ASJC Scopus subject areas

General Neuroscience
Molecular Biology
General Biochemistry, Genetics and Molecular Biology
General Immunology and Microbiology

Access to Document

10.1038/emboj.2010.186

Cite this

Xu, D., Muniandy, P., Leo, E., Yin, J., Thangavel, S., Shen, X., Ii, M., Agama, K., Guo, R., Fox, D., Meetei, A. R., Wilson, L., Nguyen, H., Weng, N. P., Brill, S. J., Li, L., Vindigni, A., Pommier, Y., Seidman, M., & Wang, W. (2010). Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication. EMBO Journal, 29(18), 3140-3155. https://doi.org/10.1038/emboj.2010.186

Xu, D, Muniandy, P, Leo, E, Yin, J, Thangavel, S, Shen, X, Ii, M, Agama, K, Guo, R, Fox, D, Meetei, AR, Wilson, L, Nguyen, H, Weng, NP, Brill, SJ, Li, L, Vindigni, A, Pommier, Y, Seidman, M & Wang, W 2010, 'Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication', EMBO Journal, vol. 29, no. 18, pp. 3140-3155. https://doi.org/10.1038/emboj.2010.186

@article{f1901e1a469d41d0bfe27a8fe0f67528,

title = "Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication",

abstract = "BLM, the helicase defective in Bloom syndrome, is part of a multiprotein complex that protects genome stability. Here, we show that Rif1 is a novel component of the BLM complex and works with BLM to promote recovery of stalled replication forks. First, Rif1 physically interacts with the BLM complex through a conserved C-terminal domain, and the stability of Rif1 depends on the presence of the BLM complex. Second, Rif1 and BLM are recruited with similar kinetics to stalled replication forks, and the Rif1 recruitment is delayed in BLM-deficient cells. Third, genetic analyses in vertebrate DT40 cells suggest that BLM and Rif1 work in a common pathway to resist replication stress and promote recovery of stalled forks. Importantly, vertebrate Rif1 contains a DNA-binding domain that resembles the {\^I} ±CTD domain of bacterial RNA polymerase {\^I} ±; and this domain preferentially binds fork and Holliday junction (HJ) DNA in vitro and is required for Rif1 to resist replication stress in vivo. Our data suggest that Rif1 provides a new DNA-binding interface for the BLM complex to restart stalled replication forks.",

keywords = "BLM, Bloom syndrome, RMI, Rif1, replication",

author = "Dongyi Xu and Parameswary Muniandy and Elisabetta Leo and Jinhu Yin and Saravanabhavan Thangavel and Xi Shen and Miki Ii and Keli Agama and Rong Guo and David Fox and Meetei, {Amom Ruhikanta} and Lauren Wilson and Huy Nguyen and Weng, {Nan Ping} and Brill, {Steven J.} and Lei Li and Alessandro Vindigni and Yves Pommier and Michael Seidman and Weidong Wang",

year = "2010",

month = sep,

doi = "10.1038/emboj.2010.186",

language = "English (US)",

volume = "29",

pages = "3140--3155",

journal = "EMBO Journal",

issn = "0261-4189",

publisher = "Nature Publishing Group",

number = "18",

}

TY - JOUR

T1 - Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication

AU - Xu, Dongyi

AU - Muniandy, Parameswary

AU - Leo, Elisabetta

AU - Yin, Jinhu

AU - Thangavel, Saravanabhavan

AU - Shen, Xi

AU - Ii, Miki

AU - Agama, Keli

AU - Guo, Rong

AU - Fox, David

AU - Meetei, Amom Ruhikanta

AU - Wilson, Lauren

AU - Nguyen, Huy

AU - Weng, Nan Ping

AU - Brill, Steven J.

AU - Li, Lei

AU - Vindigni, Alessandro

AU - Pommier, Yves

AU - Seidman, Michael

AU - Wang, Weidong

PY - 2010/9

Y1 - 2010/9

N2 - BLM, the helicase defective in Bloom syndrome, is part of a multiprotein complex that protects genome stability. Here, we show that Rif1 is a novel component of the BLM complex and works with BLM to promote recovery of stalled replication forks. First, Rif1 physically interacts with the BLM complex through a conserved C-terminal domain, and the stability of Rif1 depends on the presence of the BLM complex. Second, Rif1 and BLM are recruited with similar kinetics to stalled replication forks, and the Rif1 recruitment is delayed in BLM-deficient cells. Third, genetic analyses in vertebrate DT40 cells suggest that BLM and Rif1 work in a common pathway to resist replication stress and promote recovery of stalled forks. Importantly, vertebrate Rif1 contains a DNA-binding domain that resembles the Î ±CTD domain of bacterial RNA polymerase Î ±; and this domain preferentially binds fork and Holliday junction (HJ) DNA in vitro and is required for Rif1 to resist replication stress in vivo. Our data suggest that Rif1 provides a new DNA-binding interface for the BLM complex to restart stalled replication forks.

AB - BLM, the helicase defective in Bloom syndrome, is part of a multiprotein complex that protects genome stability. Here, we show that Rif1 is a novel component of the BLM complex and works with BLM to promote recovery of stalled replication forks. First, Rif1 physically interacts with the BLM complex through a conserved C-terminal domain, and the stability of Rif1 depends on the presence of the BLM complex. Second, Rif1 and BLM are recruited with similar kinetics to stalled replication forks, and the Rif1 recruitment is delayed in BLM-deficient cells. Third, genetic analyses in vertebrate DT40 cells suggest that BLM and Rif1 work in a common pathway to resist replication stress and promote recovery of stalled forks. Importantly, vertebrate Rif1 contains a DNA-binding domain that resembles the Î ±CTD domain of bacterial RNA polymerase Î ±; and this domain preferentially binds fork and Holliday junction (HJ) DNA in vitro and is required for Rif1 to resist replication stress in vivo. Our data suggest that Rif1 provides a new DNA-binding interface for the BLM complex to restart stalled replication forks.

KW - BLM

KW - Bloom syndrome

KW - RMI

KW - Rif1

KW - replication

UR - http://www.scopus.com/inward/record.url?scp=77956886919&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=77956886919&partnerID=8YFLogxK

U2 - 10.1038/emboj.2010.186

DO - 10.1038/emboj.2010.186

M3 - Article

C2 - 20711169

AN - SCOPUS:77956886919

SN - 0261-4189

VL - 29

SP - 3140

EP - 3155

JO - EMBO Journal

JF - EMBO Journal

IS - 18

ER -

Rif1 provides a new DNA-binding interface for the Bloom syndrome complex to maintain normal replication

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this