Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import

Veronica Rodriguez-Bravo; Raffaella Pippa; Won Min Song; Marc Carceles-Cordon; Ana Dominguez-Andres; Naoto Fujiwara; Jungreem Woo; Anna P. Koh; Adam Ertel; Ravi K. Lokareddy; Alvaro Cuesta-Dominguez; Rosa S. Kim; Irene Rodriguez-Fernandez; Peiyao Li; Ronald Gordon; Hadassa Hirschfield; Josep M. Prats; E. Premkumar Reddy; Alessandro Fatatis; Daniel P. Petrylak; Leonard Gomella; W. Kevin Kelly; Scott W. Lowe; Karen E. Knudsen; Matthew D. Galsky; Gino Cingolani; Amaia Lujambio; Yujin Hoshida; Josep Domingo-Domenech

doi:10.1016/j.cell.2018.07.015

Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import

Veronica Rodriguez-Bravo, Raffaella Pippa, Won Min Song, Marc Carceles-Cordon, Ana Dominguez-Andres, Naoto Fujiwara, Jungreem Woo, Anna P. Koh, Adam Ertel, Ravi K. Lokareddy, Alvaro Cuesta-Dominguez, Rosa S. Kim, Irene Rodriguez-Fernandez, Peiyao Li, Ronald Gordon, Hadassa Hirschfield, Josep M. Prats, E. Premkumar Reddy, Alessandro Fatatis, Daniel P. PetrylakLeonard Gomella, W. Kevin Kelly, Scott W. Lowe, Karen E. Knudsen, Matthew D. Galsky, Gino Cingolani, Amaia Lujambio, Yujin Hoshida, Josep Domingo-Domenech

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

80 Scopus citations

Abstract

Nuclear pore complexes (NPCs) regulate nuclear-cytoplasmic transport, transcription, and genome integrity in eukaryotic cells. However, their functional roles in cancer remain poorly understood. We interrogated the evolutionary transcriptomic landscape of NPC components, nucleoporins (Nups), from primary to advanced metastatic human prostate cancer (PC). Focused loss-of-function genetic screen of top-upregulated Nups in aggressive PC models identified POM121 as a key contributor to PC aggressiveness. Mechanistically, POM121 promoted PC progression by enhancing importin-dependent nuclear transport of key oncogenic (E2F1, MYC) and PC-specific (AR-GATA2) transcription factors, uncovering a pharmacologically targetable axis that, when inhibited, decreased tumor growth, restored standard therapy efficacy, and improved survival in patient-derived pre-clinical models. Our studies molecularly establish a role of NPCs in PC progression and give a rationale for NPC-regulated nuclear import targeting as a therapeutic strategy for lethal PC. These findings may have implications for understanding how NPC deregulation contributes to the pathogenesis of other tumor types. POM121- and importin β-mediated nuclear import of a subset of oncogenic transcription factors promotes prostate cancer aggressiveness and reveals a pharmacologically targetable dependency.

Original language	English (US)
Pages (from-to)	1200-1215.e20
Journal	Cell
Volume	174
Issue number	5
DOIs	https://doi.org/10.1016/j.cell.2018.07.015
State	Published - Aug 23 2018

Keywords

E2F1
GATA2
MYC
POM121
androgen receptor
importin β
nuclear import
nuclear pore
nuclear transport
prostate cancer

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

Access to Document

10.1016/j.cell.2018.07.015

Cite this

Rodriguez-Bravo, V., Pippa, R., Song, W. M., Carceles-Cordon, M., Dominguez-Andres, A., Fujiwara, N., Woo, J., Koh, A. P., Ertel, A., Lokareddy, R. K., Cuesta-Dominguez, A., Kim, R. S., Rodriguez-Fernandez, I., Li, P., Gordon, R., Hirschfield, H., Prats, J. M., Reddy, E. P., Fatatis, A., ... Domingo-Domenech, J. (2018). Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import. Cell, 174(5), 1200-1215.e20. https://doi.org/10.1016/j.cell.2018.07.015

Rodriguez-Bravo, V, Pippa, R, Song, WM, Carceles-Cordon, M, Dominguez-Andres, A, Fujiwara, N, Woo, J, Koh, AP, Ertel, A, Lokareddy, RK, Cuesta-Dominguez, A, Kim, RS, Rodriguez-Fernandez, I, Li, P, Gordon, R, Hirschfield, H, Prats, JM, Reddy, EP, Fatatis, A, Petrylak, DP, Gomella, L, Kelly, WK, Lowe, SW, Knudsen, KE, Galsky, MD, Cingolani, G, Lujambio, A, Hoshida, Y & Domingo-Domenech, J 2018, 'Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import', Cell, vol. 174, no. 5, pp. 1200-1215.e20. https://doi.org/10.1016/j.cell.2018.07.015

@article{19b0c97ee8c04a5cab270f8660214b43,

title = "Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import",

abstract = "Nuclear pore complexes (NPCs) regulate nuclear-cytoplasmic transport, transcription, and genome integrity in eukaryotic cells. However, their functional roles in cancer remain poorly understood. We interrogated the evolutionary transcriptomic landscape of NPC components, nucleoporins (Nups), from primary to advanced metastatic human prostate cancer (PC). Focused loss-of-function genetic screen of top-upregulated Nups in aggressive PC models identified POM121 as a key contributor to PC aggressiveness. Mechanistically, POM121 promoted PC progression by enhancing importin-dependent nuclear transport of key oncogenic (E2F1, MYC) and PC-specific (AR-GATA2) transcription factors, uncovering a pharmacologically targetable axis that, when inhibited, decreased tumor growth, restored standard therapy efficacy, and improved survival in patient-derived pre-clinical models. Our studies molecularly establish a role of NPCs in PC progression and give a rationale for NPC-regulated nuclear import targeting as a therapeutic strategy for lethal PC. These findings may have implications for understanding how NPC deregulation contributes to the pathogenesis of other tumor types. POM121- and importin β-mediated nuclear import of a subset of oncogenic transcription factors promotes prostate cancer aggressiveness and reveals a pharmacologically targetable dependency.",

keywords = "E2F1, GATA2, MYC, POM121, androgen receptor, importin β, nuclear import, nuclear pore, nuclear transport, prostate cancer",

author = "Veronica Rodriguez-Bravo and Raffaella Pippa and Song, {Won Min} and Marc Carceles-Cordon and Ana Dominguez-Andres and Naoto Fujiwara and Jungreem Woo and Koh, {Anna P.} and Adam Ertel and Lokareddy, {Ravi K.} and Alvaro Cuesta-Dominguez and Kim, {Rosa S.} and Irene Rodriguez-Fernandez and Peiyao Li and Ronald Gordon and Hadassa Hirschfield and Prats, {Josep M.} and Reddy, {E. Premkumar} and Alessandro Fatatis and Petrylak, {Daniel P.} and Leonard Gomella and Kelly, {W. Kevin} and Lowe, {Scott W.} and Knudsen, {Karen E.} and Galsky, {Matthew D.} and Gino Cingolani and Amaia Lujambio and Yujin Hoshida and Josep Domingo-Domenech",

note = "Funding Information: V.R.-B. is supported by NIH/NCI grant K22 CA207458. A.L. is supported by DoD grants CA150272P2 and CA150178. Y.H. is supported by the NIH/NCI grant R01 DK099558, E.U. ERC-2014-AdG-671231 HEPCIR, and DoD W81XWH-16-1-0363. J.D.-D. is supported by NIH/NCI grant R01 CA207311. Funding Information: V.R.-B. is supported by NIH/NCI grant K22 CA207458 . A.L. is supported by DoD grants CA150272P2 and CA150178 . Y.H. is supported by the NIH/NCI grant R01 DK099558 , E.U. ERC-2014-AdG-671231 HEPCIR , and DoD W81XWH-16-1-0363 . J.D.-D. is supported by NIH/NCI grant R01 CA207311 . Publisher Copyright: {\textcopyright} 2018 Elsevier Inc.",

year = "2018",

month = aug,

day = "23",

doi = "10.1016/j.cell.2018.07.015",

language = "English (US)",

volume = "174",

pages = "1200--1215.e20",

journal = "Cell",

issn = "0092-8674",

publisher = "Cell Press",

number = "5",

}

TY - JOUR

T1 - Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import

AU - Rodriguez-Bravo, Veronica

AU - Pippa, Raffaella

AU - Song, Won Min

AU - Carceles-Cordon, Marc

AU - Dominguez-Andres, Ana

AU - Fujiwara, Naoto

AU - Woo, Jungreem

AU - Koh, Anna P.

AU - Ertel, Adam

AU - Lokareddy, Ravi K.

AU - Cuesta-Dominguez, Alvaro

AU - Kim, Rosa S.

AU - Rodriguez-Fernandez, Irene

AU - Li, Peiyao

AU - Gordon, Ronald

AU - Hirschfield, Hadassa

AU - Prats, Josep M.

AU - Reddy, E. Premkumar

AU - Fatatis, Alessandro

AU - Petrylak, Daniel P.

AU - Gomella, Leonard

AU - Kelly, W. Kevin

AU - Lowe, Scott W.

AU - Knudsen, Karen E.

AU - Galsky, Matthew D.

AU - Cingolani, Gino

AU - Lujambio, Amaia

AU - Hoshida, Yujin

AU - Domingo-Domenech, Josep

N1 - Funding Information: V.R.-B. is supported by NIH/NCI grant K22 CA207458. A.L. is supported by DoD grants CA150272P2 and CA150178. Y.H. is supported by the NIH/NCI grant R01 DK099558, E.U. ERC-2014-AdG-671231 HEPCIR, and DoD W81XWH-16-1-0363. J.D.-D. is supported by NIH/NCI grant R01 CA207311. Funding Information: V.R.-B. is supported by NIH/NCI grant K22 CA207458 . A.L. is supported by DoD grants CA150272P2 and CA150178 . Y.H. is supported by the NIH/NCI grant R01 DK099558 , E.U. ERC-2014-AdG-671231 HEPCIR , and DoD W81XWH-16-1-0363 . J.D.-D. is supported by NIH/NCI grant R01 CA207311 . Publisher Copyright: © 2018 Elsevier Inc.

PY - 2018/8/23

Y1 - 2018/8/23

N2 - Nuclear pore complexes (NPCs) regulate nuclear-cytoplasmic transport, transcription, and genome integrity in eukaryotic cells. However, their functional roles in cancer remain poorly understood. We interrogated the evolutionary transcriptomic landscape of NPC components, nucleoporins (Nups), from primary to advanced metastatic human prostate cancer (PC). Focused loss-of-function genetic screen of top-upregulated Nups in aggressive PC models identified POM121 as a key contributor to PC aggressiveness. Mechanistically, POM121 promoted PC progression by enhancing importin-dependent nuclear transport of key oncogenic (E2F1, MYC) and PC-specific (AR-GATA2) transcription factors, uncovering a pharmacologically targetable axis that, when inhibited, decreased tumor growth, restored standard therapy efficacy, and improved survival in patient-derived pre-clinical models. Our studies molecularly establish a role of NPCs in PC progression and give a rationale for NPC-regulated nuclear import targeting as a therapeutic strategy for lethal PC. These findings may have implications for understanding how NPC deregulation contributes to the pathogenesis of other tumor types. POM121- and importin β-mediated nuclear import of a subset of oncogenic transcription factors promotes prostate cancer aggressiveness and reveals a pharmacologically targetable dependency.

AB - Nuclear pore complexes (NPCs) regulate nuclear-cytoplasmic transport, transcription, and genome integrity in eukaryotic cells. However, their functional roles in cancer remain poorly understood. We interrogated the evolutionary transcriptomic landscape of NPC components, nucleoporins (Nups), from primary to advanced metastatic human prostate cancer (PC). Focused loss-of-function genetic screen of top-upregulated Nups in aggressive PC models identified POM121 as a key contributor to PC aggressiveness. Mechanistically, POM121 promoted PC progression by enhancing importin-dependent nuclear transport of key oncogenic (E2F1, MYC) and PC-specific (AR-GATA2) transcription factors, uncovering a pharmacologically targetable axis that, when inhibited, decreased tumor growth, restored standard therapy efficacy, and improved survival in patient-derived pre-clinical models. Our studies molecularly establish a role of NPCs in PC progression and give a rationale for NPC-regulated nuclear import targeting as a therapeutic strategy for lethal PC. These findings may have implications for understanding how NPC deregulation contributes to the pathogenesis of other tumor types. POM121- and importin β-mediated nuclear import of a subset of oncogenic transcription factors promotes prostate cancer aggressiveness and reveals a pharmacologically targetable dependency.

KW - E2F1

KW - GATA2

KW - MYC

KW - POM121

KW - androgen receptor

KW - importin β

KW - nuclear import

KW - nuclear pore

KW - nuclear transport

KW - prostate cancer

UR - http://www.scopus.com/inward/record.url?scp=85053121228&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85053121228&partnerID=8YFLogxK

U2 - 10.1016/j.cell.2018.07.015

DO - 10.1016/j.cell.2018.07.015

M3 - Article

C2 - 30100187

AN - SCOPUS:85053121228

SN - 0092-8674

VL - 174

SP - 1200-1215.e20

JO - Cell

JF - Cell

IS - 5

ER -

Nuclear Pores Promote Lethal Prostate Cancer by Increasing POM121-Driven E2F1, MYC, and AR Nuclear Import

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this