A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer

Shane Stegeman; Ernest Amankwah; Kerenaftali Klein; Tracy A. O’Mara; Donghwa Kim; Hui Yi Lin; Jennifer Permuth-Wey; Thomas A. Sellers; Srilakshmi Srinivasan; Rosalind Eeles; The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium; Australian Prostate Cancer BioResource; Jyotsna Batra

doi:10.1158/2159-8290.CD-14-1057

A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer

Shane Stegeman
, Ernest Amankwah
, Kerenaftali Klein
, Tracy A. O’Mara
, Donghwa Kim
, Hui Yi Lin
, Jennifer Permuth-Wey
, Thomas A. Sellers
, Srilakshmi Srinivasan
, Rosalind Eeles
, The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium
, Australian Prostate Cancer BioResource
, Jyotsna Batra

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

Abstract

Prostate cancer is the second most common malignancy among men worldwide. Genome-wide association studies have identified 100 risk variants for prostate cancer, which can explain approximately 33% of the familial risk of the disease. We hypothesized that a comprehensive analysis of genetic variations found within the 3′ untranslated region of genes predicted to affect miRNA binding (miRSNP) can identify additional prostate cancer risk variants. We investigated the association between 2,169 miRSNPs and prostate cancer risk in a large-scale analysis of 22,301 cases and 22,320 controls of European ancestry from 23 participating studies. Twenty-two miRSNPs were associated (P < 2.3 × 10^-5) with risk of prostate cancer, 10 of which were within 7 genes previously not mapped by GWAS studies. Further, using miRNA mimics and reporter gene assays, we showed that miR-3162-5p has specific affinity for the KLK3 rs1058205 miRSNP T-allele, whereas miR-370 has greater affinity for the VAMP8 rs1010 miRSNP A-allele, validating their functional role.

SIGNIFICANCE: Findings from this large association study suggest that a focus on miRSNPs, including functional evaluation, can identify candidate risk loci below currently accepted statistical levels of genome-wide significance. Studies of miRNAs and their interactions with SNPs could provide further insights into the mechanisms of prostate cancer risk.

Original language	English
Pages (from-to)	368-379
Number of pages	12
Journal	Cancer Discovery
Volume	5
Issue number	4
DOIs	https://doi.org/10.1158/2159-8290.CD-14-1057
Publication status	Published - 1 Apr 2015
Externally published	Yes

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Stegeman, S., Amankwah, E., Klein, K., O’Mara, T. A., Kim, D., Lin, H. Y., Permuth-Wey, J., Sellers, T. A., Srinivasan, S., Eeles, R., The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium, Australian Prostate Cancer BioResource, & Batra, J. (2015). A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer. Cancer Discovery, 5(4), 368-379. https://doi.org/10.1158/2159-8290.CD-14-1057

@article{a6c5ec9e6ebd4b1081be302ae901506d,

title = "A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer",

abstract = "Prostate cancer is the second most common malignancy among men worldwide. Genome-wide association studies have identified 100 risk variants for prostate cancer, which can explain approximately 33\% of the familial risk of the disease. We hypothesized that a comprehensive analysis of genetic variations found within the 3′ untranslated region of genes predicted to affect miRNA binding (miRSNP) can identify additional prostate cancer risk variants. We investigated the association between 2,169 miRSNPs and prostate cancer risk in a large-scale analysis of 22,301 cases and 22,320 controls of European ancestry from 23 participating studies. Twenty-two miRSNPs were associated (P < 2.3 × 10-5) with risk of prostate cancer, 10 of which were within 7 genes previously not mapped by GWAS studies. Further, using miRNA mimics and reporter gene assays, we showed that miR-3162-5p has specific affinity for the KLK3 rs1058205 miRSNP T-allele, whereas miR-370 has greater affinity for the VAMP8 rs1010 miRSNP A-allele, validating their functional role. SIGNIFICANCE: Findings from this large association study suggest that a focus on miRSNPs, including functional evaluation, can identify candidate risk loci below currently accepted statistical levels of genome-wide significance. Studies of miRNAs and their interactions with SNPs could provide further insights into the mechanisms of prostate cancer risk.",

author = "Shane Stegeman and Ernest Amankwah and Kerenaftali Klein and O{\textquoteright}Mara, \{Tracy A.\} and Donghwa Kim and Lin, \{Hui Yi\} and Jennifer Permuth-Wey and Sellers, \{Thomas A.\} and Srilakshmi Srinivasan and Rosalind Eeles and \{The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium\} and \{Australian Prostate Cancer BioResource\} and Doug Easton and Zsofia Kote-Jarai and \{Al Olama\}, \{Ali Amin\} and Sara Benlloch and Kenneth Muir and Giles, \{Graham G.\} and Fredrik Wiklund and Henrik Gronberg and Haiman, \{Christopher A.\} and Johanna Schleutker and Nordestgaard, \{B{\o}rge G.\} and Travis, \{Ruth C.\} and David Neal and Paul Pharoah and Khaw, \{Kay Tee\} and Stanford, \{Janet L.\} and Blot, \{William J.\} and Stephen Thibodeau and Christiane Maier and Kibel, \{Adam S.\} and Cezary Cybulski and Lisa Cannon-Albright and Hermann Brenner and Radka Kaneva and Teixeira, \{Manuel R.\} and Spurdle, \{Amanda B.\} and Clements, \{Judith A.\} and Park, \{Jong Y.\} and Jyotsna Batra and Margaret Cook and Angela Morgan and Artitaya Lophatananon and Cyril Fisher and Daniel Leongamornlert and Saunders, \{Edward J.\} and Sawyer, \{Emma J.\} and Koveela Govindasami and Malgorzata Tymrakiewicz and Michelle Guy and Naomi Livni and Rosemary Wilkinson and Sara Jugurnauth-Little and Steve Hazel and Tokhir Dadaev and John Pedersen and Hopper, \{John L.\} and Southey, \{Melissa C.\} and Ami Karlsson and Carin Cavalli-Bjoerkman and Johansson, \{Jan Erik\} and Jan Adolfson and Markus Aly and Michael Broms and Paer Stattin and Henderson, \{Brian E.\} and Fredrick Schumacher and Anssi Auvinen and Kimmo Taari and Liisa Maeaettaenen and Paula Kujala and Teemu Murtola and Tammela, \{Teuvo L.J.\} and Tiina Wahlfors and Andreas Roder and Peter Iversen and Peter Klarskov and Nielsen, \{Sune F.\} and Maren Weischer and Key, \{Tim J.\} and Hans Wallinder and Sven Gustafsson and Donovan, \{Jenny L.\} and Freddie Hamdy and Anne George and Athene Lane and Gemma Marsden and Michael Davis and Paul Brown and Nora Pashayan and Sarah Holt and Signorello, \{Lisa B.\} and Wei Zheng and Liang Wang and Lori Tillmans and Shaun Riska and Antje Rinckleb and Kathleen Herkommer and Manuel Luedeke",

year = "2015",

month = apr,

day = "1",

doi = "10.1158/2159-8290.CD-14-1057",

language = "English",

volume = "5",

pages = "368--379",

journal = "Cancer Discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "4",

}

Stegeman, S, Amankwah, E, Klein, K, O’Mara, TA, Kim, D, Lin, HY, Permuth-Wey, J, Sellers, TA, Srinivasan, S, Eeles, R, The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium, Australian Prostate Cancer BioResource & Batra, J 2015, 'A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer', Cancer Discovery, vol. 5, no. 4, pp. 368-379. https://doi.org/10.1158/2159-8290.CD-14-1057

TY - JOUR

T1 - A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer

AU - Stegeman, Shane

AU - Amankwah, Ernest

AU - Klein, Kerenaftali

AU - O’Mara, Tracy A.

AU - Kim, Donghwa

AU - Lin, Hui Yi

AU - Permuth-Wey, Jennifer

AU - Sellers, Thomas A.

AU - Srinivasan, Srilakshmi

AU - Eeles, Rosalind

AU - The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium

AU - Australian Prostate Cancer BioResource

AU - Easton, Doug

AU - Kote-Jarai, Zsofia

AU - Al Olama, Ali Amin

AU - Benlloch, Sara

AU - Muir, Kenneth

AU - Giles, Graham G.

AU - Wiklund, Fredrik

AU - Gronberg, Henrik

AU - Haiman, Christopher A.

AU - Schleutker, Johanna

AU - Nordestgaard, Børge G.

AU - Travis, Ruth C.

AU - Neal, David

AU - Pharoah, Paul

AU - Khaw, Kay Tee

AU - Stanford, Janet L.

AU - Blot, William J.

AU - Thibodeau, Stephen

AU - Maier, Christiane

AU - Kibel, Adam S.

AU - Cybulski, Cezary

AU - Cannon-Albright, Lisa

AU - Brenner, Hermann

AU - Kaneva, Radka

AU - Teixeira, Manuel R.

AU - Spurdle, Amanda B.

AU - Clements, Judith A.

AU - Park, Jong Y.

AU - Batra, Jyotsna

AU - Cook, Margaret

AU - Morgan, Angela

AU - Lophatananon, Artitaya

AU - Fisher, Cyril

AU - Leongamornlert, Daniel

AU - Saunders, Edward J.

AU - Sawyer, Emma J.

AU - Govindasami, Koveela

AU - Tymrakiewicz, Malgorzata

AU - Guy, Michelle

AU - Livni, Naomi

AU - Wilkinson, Rosemary

AU - Jugurnauth-Little, Sara

AU - Hazel, Steve

AU - Dadaev, Tokhir

AU - Pedersen, John

AU - Hopper, John L.

AU - Southey, Melissa C.

AU - Karlsson, Ami

AU - Cavalli-Bjoerkman, Carin

AU - Johansson, Jan Erik

AU - Adolfson, Jan

AU - Aly, Markus

AU - Broms, Michael

AU - Stattin, Paer

AU - Henderson, Brian E.

AU - Schumacher, Fredrick

AU - Auvinen, Anssi

AU - Taari, Kimmo

AU - Maeaettaenen, Liisa

AU - Kujala, Paula

AU - Murtola, Teemu

AU - Tammela, Teuvo L.J.

AU - Wahlfors, Tiina

AU - Roder, Andreas

AU - Iversen, Peter

AU - Klarskov, Peter

AU - Nielsen, Sune F.

AU - Weischer, Maren

AU - Key, Tim J.

AU - Wallinder, Hans

AU - Gustafsson, Sven

AU - Donovan, Jenny L.

AU - Hamdy, Freddie

AU - George, Anne

AU - Lane, Athene

AU - Marsden, Gemma

AU - Davis, Michael

AU - Brown, Paul

AU - Pashayan, Nora

AU - Holt, Sarah

AU - Signorello, Lisa B.

AU - Zheng, Wei

AU - Wang, Liang

AU - Tillmans, Lori

AU - Riska, Shaun

AU - Rinckleb, Antje

AU - Herkommer, Kathleen

AU - Luedeke, Manuel

PY - 2015/4/1

Y1 - 2015/4/1

N2 - Prostate cancer is the second most common malignancy among men worldwide. Genome-wide association studies have identified 100 risk variants for prostate cancer, which can explain approximately 33% of the familial risk of the disease. We hypothesized that a comprehensive analysis of genetic variations found within the 3′ untranslated region of genes predicted to affect miRNA binding (miRSNP) can identify additional prostate cancer risk variants. We investigated the association between 2,169 miRSNPs and prostate cancer risk in a large-scale analysis of 22,301 cases and 22,320 controls of European ancestry from 23 participating studies. Twenty-two miRSNPs were associated (P < 2.3 × 10-5) with risk of prostate cancer, 10 of which were within 7 genes previously not mapped by GWAS studies. Further, using miRNA mimics and reporter gene assays, we showed that miR-3162-5p has specific affinity for the KLK3 rs1058205 miRSNP T-allele, whereas miR-370 has greater affinity for the VAMP8 rs1010 miRSNP A-allele, validating their functional role. SIGNIFICANCE: Findings from this large association study suggest that a focus on miRSNPs, including functional evaluation, can identify candidate risk loci below currently accepted statistical levels of genome-wide significance. Studies of miRNAs and their interactions with SNPs could provide further insights into the mechanisms of prostate cancer risk.

AB - Prostate cancer is the second most common malignancy among men worldwide. Genome-wide association studies have identified 100 risk variants for prostate cancer, which can explain approximately 33% of the familial risk of the disease. We hypothesized that a comprehensive analysis of genetic variations found within the 3′ untranslated region of genes predicted to affect miRNA binding (miRSNP) can identify additional prostate cancer risk variants. We investigated the association between 2,169 miRSNPs and prostate cancer risk in a large-scale analysis of 22,301 cases and 22,320 controls of European ancestry from 23 participating studies. Twenty-two miRSNPs were associated (P < 2.3 × 10-5) with risk of prostate cancer, 10 of which were within 7 genes previously not mapped by GWAS studies. Further, using miRNA mimics and reporter gene assays, we showed that miR-3162-5p has specific affinity for the KLK3 rs1058205 miRSNP T-allele, whereas miR-370 has greater affinity for the VAMP8 rs1010 miRSNP A-allele, validating their functional role. SIGNIFICANCE: Findings from this large association study suggest that a focus on miRSNPs, including functional evaluation, can identify candidate risk loci below currently accepted statistical levels of genome-wide significance. Studies of miRNAs and their interactions with SNPs could provide further insights into the mechanisms of prostate cancer risk.

UR - https://www.scopus.com/pages/publications/85000352081

U2 - 10.1158/2159-8290.CD-14-1057

DO - 10.1158/2159-8290.CD-14-1057

M3 - Article

C2 - 25691096

AN - SCOPUS:85000352081

SN - 2159-8274

VL - 5

SP - 368

EP - 379

JO - Cancer Discovery

JF - Cancer Discovery

IS - 4

ER -

A large-scale analysis of genetic variants within putative miRNA binding sites in prostate cancer

Abstract

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