Systematic screening reveals a role for BRCA1 in the response to transcription-associated DNA damage

Sarah J. Hill; Thomas Rolland; Guillaume Adelmant; Xianfang Xia; Matthew S. Owen; Amélie Dricot; Travis I. Zack; Nidhi Sahni; Yves Jacob; Tong Hao; Kristine M. McKinney; Allison P. Clark; Deepak Reyon; Shengdar Q. Tsai; J. Keith Joung; Rameen Beroukhim; Jarrod A. Marto; Marc Vidal; Suzanne Gaudet; David E. Hill; David M. Livingston

doi:10.1101/gad.241620.114

Systematic screening reveals a role for BRCA1 in the response to transcription-associated DNA damage

Sarah J. Hill, Thomas Rolland, Guillaume Adelmant, Xianfang Xia, Matthew S. Owen, Amélie Dricot, Travis I. Zack, Nidhi Sahni, Yves Jacob, Tong Hao, Kristine M. McKinney, Allison P. Clark, Deepak Reyon, Shengdar Q. Tsai, J. Keith Joung, Rameen Beroukhim, Jarrod A. Marto, Marc Vidal, Suzanne Gaudet, David E. HillDavid M. Livingston

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76 Scopus citations

Abstract

BRCA1 is a breast and ovarian tumor suppressor. Given its numerous incompletely understood functions and the possibility that more exist, we performed complementary systematic screens in search of new BRCA1 protein-interacting partners. New BRCA1 functions and/or a better understanding of existing ones were sought. Among the new interacting proteins identified, genetic interactions were detected between BRCA1 and four of the interactors: TONSL, SETX, TCEANC, and TCEA2. Genetic interactions were also detected between BRCA1 and certain interactors of TONSL, including both members of the FACT complex. From these results, a new BRCA1 function in the response to transcription-associated DNA damage was detected. Specifically, new roles for BRCA1 in the restart of transcription after UV damage and in preventing or repairing damage caused by stabilized R loops were identified. These roles are likely carried out together with some of the newly identified interactors. This new function may be important in BRCA1 tumor suppression, since the expression of several interactors, including some of the above-noted transcription proteins, is repeatedly aberrant in both breast and ovarian cancers.

Original language	English (US)
Pages (from-to)	1957-1975
Number of pages	19
Journal	Genes and Development
Volume	28
Issue number	17
DOIs	https://doi.org/10.1101/gad.241620.114
State	Published - Sep 1 2014
Externally published	Yes

Keywords

BRCA1 interaction screening
DNA damage
Transcription

ASJC Scopus subject areas

Genetics
Developmental Biology

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10.1101/gad.241620.114

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Hill, S. J., Rolland, T., Adelmant, G., Xia, X., Owen, M. S., Dricot, A., Zack, T. I., Sahni, N., Jacob, Y., Hao, T., McKinney, K. M., Clark, A. P., Reyon, D., Tsai, S. Q., Joung, J. K., Beroukhim, R., Marto, J. A., Vidal, M., Gaudet, S., ... Livingston, D. M. (2014). Systematic screening reveals a role for BRCA1 in the response to transcription-associated DNA damage. Genes and Development, 28(17), 1957-1975. https://doi.org/10.1101/gad.241620.114

Hill, SJ, Rolland, T, Adelmant, G, Xia, X, Owen, MS, Dricot, A, Zack, TI, Sahni, N, Jacob, Y, Hao, T, McKinney, KM, Clark, AP, Reyon, D, Tsai, SQ, Joung, JK, Beroukhim, R, Marto, JA, Vidal, M, Gaudet, S, Hill, DE & Livingston, DM 2014, 'Systematic screening reveals a role for BRCA1 in the response to transcription-associated DNA damage', Genes and Development, vol. 28, no. 17, pp. 1957-1975. https://doi.org/10.1101/gad.241620.114

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abstract = "BRCA1 is a breast and ovarian tumor suppressor. Given its numerous incompletely understood functions and the possibility that more exist, we performed complementary systematic screens in search of new BRCA1 protein-interacting partners. New BRCA1 functions and/or a better understanding of existing ones were sought. Among the new interacting proteins identified, genetic interactions were detected between BRCA1 and four of the interactors: TONSL, SETX, TCEANC, and TCEA2. Genetic interactions were also detected between BRCA1 and certain interactors of TONSL, including both members of the FACT complex. From these results, a new BRCA1 function in the response to transcription-associated DNA damage was detected. Specifically, new roles for BRCA1 in the restart of transcription after UV damage and in preventing or repairing damage caused by stabilized R loops were identified. These roles are likely carried out together with some of the newly identified interactors. This new function may be important in BRCA1 tumor suppression, since the expression of several interactors, including some of the above-noted transcription proteins, is repeatedly aberrant in both breast and ovarian cancers.",

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AU - Tsai, Shengdar Q.

AU - Joung, J. Keith

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AB - BRCA1 is a breast and ovarian tumor suppressor. Given its numerous incompletely understood functions and the possibility that more exist, we performed complementary systematic screens in search of new BRCA1 protein-interacting partners. New BRCA1 functions and/or a better understanding of existing ones were sought. Among the new interacting proteins identified, genetic interactions were detected between BRCA1 and four of the interactors: TONSL, SETX, TCEANC, and TCEA2. Genetic interactions were also detected between BRCA1 and certain interactors of TONSL, including both members of the FACT complex. From these results, a new BRCA1 function in the response to transcription-associated DNA damage was detected. Specifically, new roles for BRCA1 in the restart of transcription after UV damage and in preventing or repairing damage caused by stabilized R loops were identified. These roles are likely carried out together with some of the newly identified interactors. This new function may be important in BRCA1 tumor suppression, since the expression of several interactors, including some of the above-noted transcription proteins, is repeatedly aberrant in both breast and ovarian cancers.

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Systematic screening reveals a role for BRCA1 in the response to transcription-associated DNA damage

Abstract

Keywords

ASJC Scopus subject areas

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