Synthetic lethality between androgen receptor signalling and the PARP pathway in prostate cancer

dc.date.accessioned	2018-09-06T11:02:29Z
dc.date.available	2018-09-06T11:02:29Z
dc.date.created	2018-01-04T11:07:43Z
dc.date.issued	2017
dc.identifier.citation	Asim, Mohammad Tarish, Firas Zecchini, Heather I. Sanjiv, Kumar Gelali, Eleni Massie, Charles E. Baridi, Ajoeb Warren, Anne Y. Zhao, Wanfeng Ogris, Christoph McDuffus, Leigh-Anne Mascalchi, Patrice Shaw, Greg Dev, Harveer Wadhwa, Karan Wijnhoven, Paul Forment, Josep V Lyons, Scott R Lynch, Andy G. O'Neill, Cormac Zecchini, Vincent R. Rennie, Paul S. Baniahmad, Aria Tavare, Simon Mills, Ian Geoffrey Galanty, Yaron Crosetto, Nicola Schultz, Niklas Neal, David Helleday, Thomas . Synthetic lethality between androgen receptor signalling and the PARP pathway in prostate cancer. Nature Communications. 2017, 8(1)
dc.identifier.uri	http://hdl.handle.net/10852/64163
dc.description.abstract	Emerging data demonstrate homologous recombination (HR) defects in castration-resistant prostate cancers, rendering these tumours sensitive to PARP inhibition. Here we demonstrate a direct requirement for the androgen receptor (AR) to maintain HR gene expression and HR activity in prostate cancer. We show that PARP-mediated repair pathways are upregulated in prostate cancer following androgen-deprivation therapy (ADT). Furthermore, upregulation of PARP activity is essential for the survival of prostate cancer cells and we demonstrate a synthetic lethality between ADT and PARP inhibition in vivo. Our data suggest that ADT can functionally impair HR prior to the development of castration resistance and that, this potentially could be exploited therapeutically using PARP inhibitors in combination with androgen-deprivation therapy upfront in advanced or high-risk prostate cancer.	en_US
dc.language	EN
dc.rights	Attribution 4.0 International
dc.rights.uri	https://creativecommons.org/licenses/by/4.0/
dc.title	Synthetic lethality between androgen receptor signalling and the PARP pathway in prostate cancer	en_US
dc.type	Journal article	en_US
dc.creator.author	Asim, Mohammad
dc.creator.author	Tarish, Firas
dc.creator.author	Zecchini, Heather I.
dc.creator.author	Sanjiv, Kumar
dc.creator.author	Gelali, Eleni
dc.creator.author	Massie, Charles E.
dc.creator.author	Baridi, Ajoeb
dc.creator.author	Warren, Anne Y.
dc.creator.author	Zhao, Wanfeng
dc.creator.author	Ogris, Christoph
dc.creator.author	McDuffus, Leigh-Anne
dc.creator.author	Mascalchi, Patrice
dc.creator.author	Shaw, Greg
dc.creator.author	Dev, Harveer
dc.creator.author	Wadhwa, Karan
dc.creator.author	Wijnhoven, Paul
dc.creator.author	Forment, Josep V
dc.creator.author	Lyons, Scott R
dc.creator.author	Lynch, Andy G.
dc.creator.author	O'Neill, Cormac
dc.creator.author	Zecchini, Vincent R.
dc.creator.author	Rennie, Paul S.
dc.creator.author	Baniahmad, Aria
dc.creator.author	Tavare, Simon
dc.creator.author	Mills, Ian Geoffrey
dc.creator.author	Galanty, Yaron
dc.creator.author	Crosetto, Nicola
dc.creator.author	Schultz, Niklas
dc.creator.author	Neal, David
dc.creator.author	Helleday, Thomas
cristin.unitcode	185,57,0,0
cristin.unitname	Norsk Senter for Molekylærmedisin
cristin.ispublished	true
cristin.fulltext	original
cristin.qualitycode	2
dc.identifier.cristin	1535603
dc.identifier.bibliographiccitation	info:ofi/fmt:kev:mtx:ctx&ctx_ver=Z39.88-2004&rft_val_fmt=info:ofi/fmt:kev:mtx:journal&rft.jtitle=Nature Communications&rft.volume=8&rft.spage=&rft.date=2017
dc.identifier.jtitle	Nature Communications
dc.identifier.volume	8
dc.identifier.issue	1
dc.identifier.doi	http://dx.doi.org/10.1038/s41467-017-00393-y
dc.identifier.urn	URN:NBN:no-66722
dc.type.document	Tidsskriftartikkel	en_US
dc.type.peerreviewed	Peer reviewed
dc.source.issn	2041-1723
dc.identifier.fulltext	Fulltext https://www.duo.uio.no/bitstream/handle/10852/64163/4/s41467-017-00393-y.pdf
dc.type.version	PublishedVersion
dc.relation.project	NFR/144182