TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells

Aruna S. Jaiswal; Arijit Dutta; Gayathri Srinivasan; Yaxia Yuan; Daohong Zhou; Montaser Shaheen; Doraid T. Sadideen; Austin Kirby; Elizabeth A. Williamson; Yogesh K. Gupta; Shaun K. Olsen; Mingjiang Xu; Eva Loranc; Pramiti Mukhopadhyay; Alexander Pertsemlidis; Alexander J.R. Bishop; Patrick Sung; Jac A. Nickoloff; Robert Hromas

doi:10.1093/nar/gkad952

TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells

Aruna S. Jaiswal
, Arijit Dutta
, Gayathri Srinivasan
, Yaxia Yuan
, Daohong Zhou
, Montaser Shaheen
, Doraid T. Sadideen
, Austin Kirby
, Elizabeth A. Williamson
, Yogesh K. Gupta
, Shaun K. Olsen
, Mingjiang Xu
, Eva Loranc
, Pramiti Mukhopadhyay
, Alexander Pertsemlidis
, Alexander J.R. Bishop
, Patrick Sung
, Jac A. Nickoloff
, Robert Hromas

Producción científica: Article › revisión exhaustiva

10 Citas (Scopus)

Resumen

BRCA1-deficient cells have increased IRE1 RNase, which degrades multiple microRNAs. Reconstituting expression of one of these, miR-4638-5p, resulted in synthetic lethality in BRCA1-deficient cancer cells. We found that miR-4638-5p represses expression of TATDN2, a poorly characterized member of the TATD nuclease family. We discovered that human TATDN2 has RNA 3′ exonuclease and endonuclease activity on double-stranded hairpin RNA structures. Given the cleavage of hairpin RNA by TATDN2, and that BRCA1-deficient cells have difficulty resolving R-loops, we tested whether TATDN2 could resolve R-loops. Using in vitro biochemical reconstitution assays, we found TATDN2 bound to R-loops and degraded the RNA strand but not DNA of multiple forms of R-loops in vitro in a Mg²⁺-dependent manner. Mutations in amino acids E593 and E705 predicted by Alphafold-2 to chelate an essential Mg²⁺ cation completely abrogated this R-loop resolution activity. Depleting TATDN2 increased cellular R-loops, DNA damage and chromosomal instability. Loss of TATDN2 resulted in poor replication fork progression in the presence of increased R-loops. Significantly, we found that TATDN2 is essential for survival of BRCA1-deficient cancer cells, but much less so for cognate BRCA1-repleted cancer cells. Thus, we propose that TATDN2 is a novel target for therapy of BRCA1-deficient cancers.

Idioma original	English (US)
Páginas (desde-hasta)	12224-12241
Número de páginas	18
Publicación	Nucleic acids research
Volumen	51
N.º	22
DOI	https://doi.org/10.1093/nar/gkad952
Estado	Published - dic 11 2023

ASJC Scopus subject areas

Genetics

Acceder al documento

10.1093/nar/gkad952

Otros archivos y enlaces

Citar esto

Jaiswal, A. S., Dutta, A., Srinivasan, G., Yuan, Y., Zhou, D., Shaheen, M., Sadideen, D. T., Kirby, A., Williamson, E. A., Gupta, Y. K., Olsen, S. K., Xu, M., Loranc, E., Mukhopadhyay, P., Pertsemlidis, A., Bishop, A. J. R., Sung, P., Nickoloff, J. A., & Hromas, R. (2023). TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells. Nucleic acids research, 51(22), 12224-12241. https://doi.org/10.1093/nar/gkad952

Jaiswal, AS, Dutta, A, Srinivasan, G, Yuan, Y , Zhou, D , Shaheen, M, Sadideen, DT, Kirby, A, Williamson, EA , Gupta, YK , Olsen, SK , Xu, M, Loranc, E, Mukhopadhyay, P, Pertsemlidis, A, Bishop, AJR, Sung, P, Nickoloff, JA & Hromas, R 2023, 'TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells', Nucleic acids research, vol. 51, n.º 22, pp. 12224-12241. https://doi.org/10.1093/nar/gkad952

@article{174c6ab3139c42be9a73f1ca722382b9,

title = "TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells",

abstract = "BRCA1-deficient cells have increased IRE1 RNase, which degrades multiple microRNAs. Reconstituting expression of one of these, miR-4638-5p, resulted in synthetic lethality in BRCA1-deficient cancer cells. We found that miR-4638-5p represses expression of TATDN2, a poorly characterized member of the TATD nuclease family. We discovered that human TATDN2 has RNA 3′ exonuclease and endonuclease activity on double-stranded hairpin RNA structures. Given the cleavage of hairpin RNA by TATDN2, and that BRCA1-deficient cells have difficulty resolving R-loops, we tested whether TATDN2 could resolve R-loops. Using in vitro biochemical reconstitution assays, we found TATDN2 bound to R-loops and degraded the RNA strand but not DNA of multiple forms of R-loops in vitro in a Mg2+-dependent manner. Mutations in amino acids E593 and E705 predicted by Alphafold-2 to chelate an essential Mg2+ cation completely abrogated this R-loop resolution activity. Depleting TATDN2 increased cellular R-loops, DNA damage and chromosomal instability. Loss of TATDN2 resulted in poor replication fork progression in the presence of increased R-loops. Significantly, we found that TATDN2 is essential for survival of BRCA1-deficient cancer cells, but much less so for cognate BRCA1-repleted cancer cells. Thus, we propose that TATDN2 is a novel target for therapy of BRCA1-deficient cancers.",

author = "Jaiswal, \{Aruna S.\} and Arijit Dutta and Gayathri Srinivasan and Yaxia Yuan and Daohong Zhou and Montaser Shaheen and Sadideen, \{Doraid T.\} and Austin Kirby and Williamson, \{Elizabeth A.\} and Gupta, \{Yogesh K.\} and Olsen, \{Shaun K.\} and Mingjiang Xu and Eva Loranc and Pramiti Mukhopadhyay and Alexander Pertsemlidis and Bishop, \{Alexander J.R.\} and Patrick Sung and Nickoloff, \{Jac A.\} and Robert Hromas",

note = "Publisher Copyright: {\textcopyright} 2023 The Author(s).",

year = "2023",

month = dec,

day = "11",

doi = "10.1093/nar/gkad952",

language = "English (US)",

volume = "51",

pages = "12224--12241",

journal = "Nucleic acids research",

issn = "0305-1048",

publisher = "Oxford University Press",

number = "22",

}

TY - JOUR

T1 - TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells

AU - Jaiswal, Aruna S.

AU - Dutta, Arijit

AU - Srinivasan, Gayathri

AU - Yuan, Yaxia

AU - Zhou, Daohong

AU - Shaheen, Montaser

AU - Sadideen, Doraid T.

AU - Kirby, Austin

AU - Williamson, Elizabeth A.

AU - Gupta, Yogesh K.

AU - Olsen, Shaun K.

AU - Xu, Mingjiang

AU - Loranc, Eva

AU - Mukhopadhyay, Pramiti

AU - Pertsemlidis, Alexander

AU - Bishop, Alexander J.R.

AU - Sung, Patrick

AU - Nickoloff, Jac A.

AU - Hromas, Robert

PY - 2023/12/11

Y1 - 2023/12/11

N2 - BRCA1-deficient cells have increased IRE1 RNase, which degrades multiple microRNAs. Reconstituting expression of one of these, miR-4638-5p, resulted in synthetic lethality in BRCA1-deficient cancer cells. We found that miR-4638-5p represses expression of TATDN2, a poorly characterized member of the TATD nuclease family. We discovered that human TATDN2 has RNA 3′ exonuclease and endonuclease activity on double-stranded hairpin RNA structures. Given the cleavage of hairpin RNA by TATDN2, and that BRCA1-deficient cells have difficulty resolving R-loops, we tested whether TATDN2 could resolve R-loops. Using in vitro biochemical reconstitution assays, we found TATDN2 bound to R-loops and degraded the RNA strand but not DNA of multiple forms of R-loops in vitro in a Mg2+-dependent manner. Mutations in amino acids E593 and E705 predicted by Alphafold-2 to chelate an essential Mg2+ cation completely abrogated this R-loop resolution activity. Depleting TATDN2 increased cellular R-loops, DNA damage and chromosomal instability. Loss of TATDN2 resulted in poor replication fork progression in the presence of increased R-loops. Significantly, we found that TATDN2 is essential for survival of BRCA1-deficient cancer cells, but much less so for cognate BRCA1-repleted cancer cells. Thus, we propose that TATDN2 is a novel target for therapy of BRCA1-deficient cancers.

AB - BRCA1-deficient cells have increased IRE1 RNase, which degrades multiple microRNAs. Reconstituting expression of one of these, miR-4638-5p, resulted in synthetic lethality in BRCA1-deficient cancer cells. We found that miR-4638-5p represses expression of TATDN2, a poorly characterized member of the TATD nuclease family. We discovered that human TATDN2 has RNA 3′ exonuclease and endonuclease activity on double-stranded hairpin RNA structures. Given the cleavage of hairpin RNA by TATDN2, and that BRCA1-deficient cells have difficulty resolving R-loops, we tested whether TATDN2 could resolve R-loops. Using in vitro biochemical reconstitution assays, we found TATDN2 bound to R-loops and degraded the RNA strand but not DNA of multiple forms of R-loops in vitro in a Mg2+-dependent manner. Mutations in amino acids E593 and E705 predicted by Alphafold-2 to chelate an essential Mg2+ cation completely abrogated this R-loop resolution activity. Depleting TATDN2 increased cellular R-loops, DNA damage and chromosomal instability. Loss of TATDN2 resulted in poor replication fork progression in the presence of increased R-loops. Significantly, we found that TATDN2 is essential for survival of BRCA1-deficient cancer cells, but much less so for cognate BRCA1-repleted cancer cells. Thus, we propose that TATDN2 is a novel target for therapy of BRCA1-deficient cancers.

UR - https://www.scopus.com/pages/publications/85179346706

UR - https://www.scopus.com/pages/publications/85179346706#tab=citedBy

U2 - 10.1093/nar/gkad952

DO - 10.1093/nar/gkad952

M3 - Article

C2 - 37953292

AN - SCOPUS:85179346706

SN - 0305-1048

VL - 51

SP - 12224

EP - 12241

JO - Nucleic acids research

JF - Nucleic acids research

IS - 22

ER -

TATDN2 resolution of R-loops is required for survival of BRCA1-mutant cancer cells

Resumen

ASJC Scopus subject areas

Acceder al documento

Otros archivos y enlaces

Huella

Citar esto