Einzeltreffer — DigiBib

Synthetic lethal screens have the potential to identify new vulnerabilities incurred by specific cancer mutations but have been hindered by lack of agreement between studies. In the case of KRAS, we identify that published synthetic lethal screen hits significantly overlap at the pathway rather than gene level. Analysis of pathways encoded as protein networks could identify synthetic lethal candidates that are more reproducible than those previously reported. Lack of overlap likely stems from biological rather than technical limitations as most synthetic lethal phenotypes are strongly modulated by changes in cellular conditions or genetic context, the latter determined using a pairwise genetic interaction map that identifies numerous interactions that suppress synthetic lethal effects. Accounting for pathway, cellular and genetic context nominates a DNA repair dependency in KRAS-mutant cells, mediated by a network containing BRCA1. We provide evidence for why most reported synthetic lethals are not reproducible which is addressable using a multi-faceted testing framework.

Titel:	Integration of multiple biological contexts reveals principles of synthetic lethality that affect reproducibility.
Autor/in / Beteiligte Person:	Ku, AA ; Hu, HM ; Zhao, X ; Shah, KN ; Kongara, S ; Wu, D ; McCormick, F ; Balmain, A ; Bandyopadhyay, S
Link:	Full Text Finder (Volltext)
Zeitschrift:	Nature communications, Jg. 11 (2020-05-12), Heft 1, S. 2375
Veröffentlichung:	[London] : Nature Pub. Group, 2020
Medientyp:	academicJournal
ISSN:	2041-1723 (electronic)
DOI:	10.1038/s41467-020-16078-y
Schlagwort:	Animals BRCA1 Protein genetics Cell Line, Tumor Computational Biology standards Disease Models, Animal Humans Mice Protein Interaction Maps genetics Proto-Oncogene Proteins p21(ras) genetics Reproducibility of Results Computational Biology methods Data Analysis Gene Regulatory Networks Neoplasms genetics Synthetic Lethal Mutations
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, N.I.H., Extramural; Research Support, Non-U.S. Gov't Language: English [Nat Commun] 2020 May 12; Vol. 11 (1), pp. 2375. <i>Date of Electronic Publication: </i>2020 May 12. MeSH Terms: Data Analysis* ; Gene Regulatory Networks* ; Synthetic Lethal Mutations* ; Computational Biology / methods ; Neoplasms / genetics ; Animals ; BRCA1 Protein / genetics ; Cell Line, Tumor ; Computational Biology / standards ; Disease Models, Animal ; Humans ; Mice ; Protein Interaction Maps / genetics ; Proto-Oncogene Proteins p21(ras) / genetics ; Reproducibility of Results References: Annu Rev Biochem. 2016 Jun 02;85:227-64. (PMID: 27145843) ; Nature. 2005 Apr 14;434(7035):917-21. (PMID: 15829967) ; Sci Transl Med. 2017 May 31;9(392):. (PMID: 28566428) ; Nature. 2005 Apr 14;434(7035):913-7. (PMID: 15829966) ; Cell. 2011 Apr 1;145(1):30-8. (PMID: 21458666) ; Cancer Res. 2011 Dec 15;71(24):7716; author reply 7717. (PMID: 22127923) ; Mol Carcinog. 1989;2(1):34-9. (PMID: 2567173) ; Cancer Res. 2006 Nov 1;66(21):10505-12. (PMID: 17079472) ; Nature. 1984 Feb 16-22;307(5952):658-60. (PMID: 6694757) ; Cancer Discov. 2015 Feb;5(2):154-67. (PMID: 25501949) ; Nat Rev Genet. 2018 Jan;19(1):34-49. (PMID: 29033457) ; Biotechniques. 2007 Aug;43(2):228-9. (PMID: 17824391) ; Trends Cancer. 2018 Oct;4(10):671-683. (PMID: 30292351) ; Nat Struct Mol Biol. 2008 Dec;15(12):1255-62. (PMID: 19011634) ; Trends Genet. 1993 Oct;9(10):362-6. (PMID: 8273152) ; Science. 2010 Jan 22;327(5964):425-31. (PMID: 20093466) ; Nucleic Acids Res. 2010 Jan;38(Database issue):D497-501. (PMID: 19884131) ; Nature. 2006 Nov 30;444(7119):638-42. (PMID: 17136094) ; Cell. 2021 May 27;184(11):3022-3040.e28. (PMID: 33961781) ; Mol Cancer Res. 2009 Aug;7(8):1244-52. (PMID: 19671679) ; Cancer Res. 2012 Nov 1;72(21):5588-99. (PMID: 23118055) ; Biotechnol Lett. 2018 Jan;40(1):5-21. (PMID: 28940015) ; Cell Res. 2012 Aug;22(8):1227-45. (PMID: 22613949) ; Cell. 2013 Oct 24;155(3):552-66. (PMID: 24243015) ; Mol Oncol. 2017 May;11(5):470-490. (PMID: 28173629) ; Nat Rev Clin Oncol. 2018 Sep;15(9):564-576. (PMID: 29955114) ; Clin Cancer Res. 2015 Apr 15;21(8):1802-9. (PMID: 25878361) ; Nature. 2008 Oct 23;455(7216):1069-75. (PMID: 18948947) ; Sci Rep. 2015 Feb 23;5:8535. (PMID: 25705018) ; Proc Natl Acad Sci U S A. 2012 Feb 21;109(8):2860-5. (PMID: 22323609) ; Cell. 2009 May 29;137(5):821-34. (PMID: 19490892) ; Genome Res. 2011 Jul;21(7):1109-21. (PMID: 21536720) ; Science. 2016 Sep 23;353(6306):. (PMID: 27708008) ; Nat Commun. 2016 Oct 11;7:13087. (PMID: 27725641) ; Oncotarget. 2017 May 23;8(21):34283-34297. (PMID: 28415695) ; Nature. 2009 Nov 5;462(7269):108-12. (PMID: 19847166) ; Nucleic Acids Res. 2013 Jan;41(Database issue):D955-61. (PMID: 23180760) ; Cancer Res. 2011 Sep 1;71(17):5818-26. (PMID: 21742770) ; Cell. 2009 May 29;137(5):835-48. (PMID: 19490893) ; PLoS One. 2016 Feb 16;11(2):e0149099. (PMID: 26881434) ; Nature. 2016 Oct 6;538(7623):114-117. (PMID: 27680702) ; Mol Syst Biol. 2019 Dec;15(12):e8831. (PMID: 31885205) ; Nat Rev Cancer. 2016 Feb;16(2):110-20. (PMID: 26775620) ; Nat Rev Drug Discov. 2017 Oct;16(10):736. (PMID: 28912598) ; Nucleic Acids Res. 2016 Jul 8;44(W1):W83-9. (PMID: 27098042) ; BMC Bioinformatics. 2003 Jan 13;4:2. (PMID: 12525261) ; Cancer Res. 2010 Dec 1;70(23):9693-702. (PMID: 21098704) ; Nat Methods. 2013 May;10(5):432-7. (PMID: 23407553) ; Science. 2010 Dec 3;330(6009):1385-9. (PMID: 21127252) ; Nat Rev Genet. 2007 Jun;8(6):437-49. (PMID: 17510664) ; Nature. 2018 Aug;560(7718):325-330. (PMID: 30089904) ; Elife. 2018 Feb 08;7:. (PMID: 29417929) ; J Thorac Oncol. 2014 Jun;9(6):784-93. (PMID: 24807155) ; Nature. 2007 Apr 12;446(7137):806-10. (PMID: 17314980) Grant Information: R35 CA210018 United States CA NCI NIH HHS; U01 CA168370 United States CA NCI NIH HHS Substance Nomenclature: 0 (BRCA1 Protein) ; 0 (BRCA1 protein, human) ; 0 (KRAS protein, human) ; EC 3.6.5.2 (Proto-Oncogene Proteins p21(ras)) Entry Date(s): Date Created: 20200514 Date Completed: 20200831 Latest Revision: 20240329 Update Code: 20240329 PubMed Central ID: PMC7217969

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Integration of multiple biological contexts reveals principles of synthetic lethality that affect reproducibility.