Analyses of germline variants associated with ovarian cancer survival identify functional candidates at the 1q22 and 19p12 outcome loci

AOCS Group; AOCS Group; On behalf of the AGO Study Group

doi:10.18632/oncotarget.18501

Analyses of germline variants associated with ovarian cancer survival identify functional candidates at the 1q22 and 19p12 outcome loci

AOCS Group, AOCS Group, On behalf of the AGO Study Group

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

4 Scopus citations

Abstract

We previously identified associations with ovarian cancer outcome at five genetic loci. To identify putatively causal genetic variants and target genes, we prioritized two ovarian outcome loci (1q22 and 19p12) for further study. Bioinformatic and functional genetic analyses indicated that MEF2D and ZNF100 are targets of candidate outcome variants at 1q22 and 19p12, respectively. At 19p12, the chromatin interaction of a putative regulatory element with the ZNF100 promoter region correlated with candidate outcome variants. At 1q22, putative regulatory elements enhanced MEF2D promoter activity and haplotypes containing candidate outcome variants modulated these effects. In a public dataset, MEF2D and ZNF100 expression were both associated with ovarian cancer progression-free or overall survival time. In an extended set of 6,162 epithelial ovarian cancer patients, we found that functional candidates at the 1q22 and 19p12 loci, as well as other regional variants, were nominally associated with patient outcome; however, no associations reached our threshold for statistical significance (p < 1×10^-5). Larger patient numbers will be needed to convincingly identify any true associations at these loci.

Original language	English (US)
Pages (from-to)	64670-64684
Number of pages	15
Journal	Oncotarget
Volume	8
Issue number	39
DOIs	https://doi.org/10.18632/oncotarget.18501
State	Published - 2017

Keywords

Gene regulation
Genetic association
Meta-analysis
Ovarian cancer outcome

ASJC Scopus subject areas

Oncology

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10.18632/oncotarget.18501

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@article{65cc3e31060c48a2958eea2fe8da60d3,

title = "Analyses of germline variants associated with ovarian cancer survival identify functional candidates at the 1q22 and 19p12 outcome loci",

abstract = "We previously identified associations with ovarian cancer outcome at five genetic loci. To identify putatively causal genetic variants and target genes, we prioritized two ovarian outcome loci (1q22 and 19p12) for further study. Bioinformatic and functional genetic analyses indicated that MEF2D and ZNF100 are targets of candidate outcome variants at 1q22 and 19p12, respectively. At 19p12, the chromatin interaction of a putative regulatory element with the ZNF100 promoter region correlated with candidate outcome variants. At 1q22, putative regulatory elements enhanced MEF2D promoter activity and haplotypes containing candidate outcome variants modulated these effects. In a public dataset, MEF2D and ZNF100 expression were both associated with ovarian cancer progression-free or overall survival time. In an extended set of 6,162 epithelial ovarian cancer patients, we found that functional candidates at the 1q22 and 19p12 loci, as well as other regional variants, were nominally associated with patient outcome; however, no associations reached our threshold for statistical significance (p < 1×10-5). Larger patient numbers will be needed to convincingly identify any true associations at these loci.",

keywords = "Gene regulation, Genetic association, Meta-analysis, Ovarian cancer outcome",

author = "{AOCS Group} and {AOCS Group} and {On behalf of the AGO Study Group} and Glubb, {Dylan M.} and Johnatty, {Sharon E.} and Quinn, {Michael C.J.} and O'Mara, {Tracy A.} and Tyrer, {Jonathan P.} and Bo Gao and Fasching, {Peter A.} and Beckmann, {Matthias W.} and Diether Lambrechts and Ignace Vergote and Edwards, {Digna R.Velez} and Alicia Beeghly-Fadiel and Javier Benitez and Garcia, {Maria J.} and Goodman, {Marc T.} and Thompson, {Pamela J.} and Thilo D{\"o}rk and Matthias D{\"u}rst and Francesmary Modungo and Kirsten Moysich and Florian Heitz and {du Bois}, Andreas and Jacobus Pfisterer and Peter Hillemanns and Karlan, {Beth Y.} and Jenny Lester and Goode, {Ellen L.} and Cunningham, {Julie M.} and Winham, {Stacey J.} and Larson, {Melissa C.} and McCauley, {Bryan M.} and Kj{\ae}r, {Susanne Kr{\"u}ger} and Allan Jensen and Schildkraut, {Joellen M.} and Andrew Berchuck and Cramer, {Daniel W.} and Terry, {Kathryn L.} and Salvesen, {Helga B.} and Line Bjorge and Webb, {Penny M.} and Peter Grant and Tanja Pejovic and Melissa Moffitt and Hogdall, {Claus K.} and Estrid Hogdall and James Paul and Rosalind Glasspool and Marcus Bernardini and Alicia Tone and David Huntsman",

note = "Publisher Copyright: {\textcopyright} Glubb et al.",

year = "2017",

doi = "10.18632/oncotarget.18501",

language = "English (US)",

volume = "8",

pages = "64670--64684",

journal = "Oncotarget",

issn = "1949-2553",

publisher = "Impact Journals",

number = "39",

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TY - JOUR

T1 - Analyses of germline variants associated with ovarian cancer survival identify functional candidates at the 1q22 and 19p12 outcome loci

AU - AOCS Group

AU - On behalf of the AGO Study Group

AU - Glubb, Dylan M.

AU - Johnatty, Sharon E.

AU - Quinn, Michael C.J.

AU - O'Mara, Tracy A.

AU - Tyrer, Jonathan P.

AU - Gao, Bo

AU - Fasching, Peter A.

AU - Beckmann, Matthias W.

AU - Lambrechts, Diether

AU - Vergote, Ignace

AU - Edwards, Digna R.Velez

AU - Beeghly-Fadiel, Alicia

AU - Benitez, Javier

AU - Garcia, Maria J.

AU - Goodman, Marc T.

AU - Thompson, Pamela J.

AU - Dörk, Thilo

AU - Dürst, Matthias

AU - Modungo, Francesmary

AU - Moysich, Kirsten

AU - Heitz, Florian

AU - du Bois, Andreas

AU - Pfisterer, Jacobus

AU - Hillemanns, Peter

AU - Karlan, Beth Y.

AU - Lester, Jenny

AU - Goode, Ellen L.

AU - Cunningham, Julie M.

AU - Winham, Stacey J.

AU - Larson, Melissa C.

AU - McCauley, Bryan M.

AU - Kjær, Susanne Krüger

AU - Jensen, Allan

AU - Schildkraut, Joellen M.

AU - Berchuck, Andrew

AU - Cramer, Daniel W.

AU - Terry, Kathryn L.

AU - Salvesen, Helga B.

AU - Bjorge, Line

AU - Webb, Penny M.

AU - Grant, Peter

AU - Pejovic, Tanja

AU - Moffitt, Melissa

AU - Hogdall, Claus K.

AU - Hogdall, Estrid

AU - Paul, James

AU - Glasspool, Rosalind

AU - Bernardini, Marcus

AU - Tone, Alicia

AU - Huntsman, David

PY - 2017

Y1 - 2017

N2 - We previously identified associations with ovarian cancer outcome at five genetic loci. To identify putatively causal genetic variants and target genes, we prioritized two ovarian outcome loci (1q22 and 19p12) for further study. Bioinformatic and functional genetic analyses indicated that MEF2D and ZNF100 are targets of candidate outcome variants at 1q22 and 19p12, respectively. At 19p12, the chromatin interaction of a putative regulatory element with the ZNF100 promoter region correlated with candidate outcome variants. At 1q22, putative regulatory elements enhanced MEF2D promoter activity and haplotypes containing candidate outcome variants modulated these effects. In a public dataset, MEF2D and ZNF100 expression were both associated with ovarian cancer progression-free or overall survival time. In an extended set of 6,162 epithelial ovarian cancer patients, we found that functional candidates at the 1q22 and 19p12 loci, as well as other regional variants, were nominally associated with patient outcome; however, no associations reached our threshold for statistical significance (p < 1×10-5). Larger patient numbers will be needed to convincingly identify any true associations at these loci.

AB - We previously identified associations with ovarian cancer outcome at five genetic loci. To identify putatively causal genetic variants and target genes, we prioritized two ovarian outcome loci (1q22 and 19p12) for further study. Bioinformatic and functional genetic analyses indicated that MEF2D and ZNF100 are targets of candidate outcome variants at 1q22 and 19p12, respectively. At 19p12, the chromatin interaction of a putative regulatory element with the ZNF100 promoter region correlated with candidate outcome variants. At 1q22, putative regulatory elements enhanced MEF2D promoter activity and haplotypes containing candidate outcome variants modulated these effects. In a public dataset, MEF2D and ZNF100 expression were both associated with ovarian cancer progression-free or overall survival time. In an extended set of 6,162 epithelial ovarian cancer patients, we found that functional candidates at the 1q22 and 19p12 loci, as well as other regional variants, were nominally associated with patient outcome; however, no associations reached our threshold for statistical significance (p < 1×10-5). Larger patient numbers will be needed to convincingly identify any true associations at these loci.

KW - Gene regulation

KW - Genetic association

KW - Meta-analysis

KW - Ovarian cancer outcome

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UR - http://www.scopus.com/inward/citedby.url?scp=85030120544&partnerID=8YFLogxK

U2 - 10.18632/oncotarget.18501

DO - 10.18632/oncotarget.18501

M3 - Article

AN - SCOPUS:85030120544

SN - 1949-2553

VL - 8

SP - 64670

EP - 64684

JO - Oncotarget

JF - Oncotarget

IS - 39

ER -

Analyses of germline variants associated with ovarian cancer survival identify functional candidates at the 1q22 and 19p12 outcome loci

Abstract

Keywords

ASJC Scopus subject areas

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