Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort

Carolina Bonilla; Sarah J. Lewis; Richard M. Martin; Jenny L. Donovan; Freddie C. Hamdy; David E. Neal; Rosalind Eeles; Doug Easton; Zsofia Kote-Jarai; Ali Amin Al Olama; The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium; Jyotsna Batra

doi:10.1186/s12916-016-0602-x

Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort

Carolina Bonilla
, Sarah J. Lewis
, Richard M. Martin^*
, Jenny L. Donovan
, Freddie C. Hamdy
, David E. Neal
, Rosalind Eeles
, Doug Easton
, Zsofia Kote-Jarai
, Ali Amin Al Olama
, The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium
, Jyotsna Batra

^*Corresponding author for this work

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

Abstract

Background:
Epidemiological studies have observed a positive association between an earlier age at sexual development and prostate cancer, but markers of sexual maturation in boys are imprecise and observational estimates are likely to suffer from a degree of uncontrolled confounding. To obtain causal estimates, we examined the role of pubertal development in prostate cancer using genetic polymorphisms associated with Tanner stage in adolescent boys in a Mendelian randomization (MR) approach.

Methods:
We derived a weighted genetic risk score for pubertal development, combining 13 SNPs associated with male Tanner stage. A higher score indicated a later puberty onset. We examined the association of this score with prostate cancer risk, stage and grade in the UK-based ProtecT case-control study (n = 2,927), and used the PRACTICAL consortium (n = 43,737) as a replication sample.

Results:
In ProtecT, the puberty genetic score was inversely associated with prostate cancer grade (odds ratio (OR) of high- vs. low-grade cancer, per tertile of the score: 0.76; 95 % CI, 0.64-0.89). In an instrumental variable estimation of the causal OR, later physical development in adolescence (equivalent to a difference of one Tanner stage between pubertal boys of the same age) was associated with a 77 % (95 % CI, 43-91 %) reduced odds of high Gleason prostate cancer. In PRACTICAL, the puberty genetic score was associated with prostate cancer stage (OR of advanced vs. localized cancer, per tertile: 0.95; 95 % CI, 0.91-1.00) and prostate cancer-specific mortality (hazard ratio amongst cases, per tertile: 0.94; 95 % CI, 0.90-0.98), but not with disease grade.

Conclusions:
Older age at sexual maturation is causally linked to a reduced risk of later prostate cancer, especially aggressive disease.

Original language	English
Article number	66
Pages (from-to)	1-11
Number of pages	11
Journal	BMC Medicine
Volume	14
Issue number	1
DOIs	https://doi.org/10.1186/s12916-016-0602-x
Publication status	Published - 1 Jan 2016
Externally published	Yes

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Pubertal development and prostate cancer risk Mendelian randomization study in a population-based cohortFinal published version, 905 KBLicence: CC BY

Cite this

Bonilla, C., Lewis, S. J., Martin, R. M., Donovan, J. L., Hamdy, F. C., Neal, D. E., Eeles, R., Easton, D., Kote-Jarai, Z., Al Olama, A. A., The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium, & Batra, J. (2016). Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort. BMC Medicine, 14(1), 1-11. Article 66. https://doi.org/10.1186/s12916-016-0602-x

@article{7a936ef160084b5b8756f71e4b5b9fed,

title = "Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort",

abstract = "Background: Epidemiological studies have observed a positive association between an earlier age at sexual development and prostate cancer, but markers of sexual maturation in boys are imprecise and observational estimates are likely to suffer from a degree of uncontrolled confounding. To obtain causal estimates, we examined the role of pubertal development in prostate cancer using genetic polymorphisms associated with Tanner stage in adolescent boys in a Mendelian randomization (MR) approach. Methods: We derived a weighted genetic risk score for pubertal development, combining 13 SNPs associated with male Tanner stage. A higher score indicated a later puberty onset. We examined the association of this score with prostate cancer risk, stage and grade in the UK-based ProtecT case-control study (n = 2,927), and used the PRACTICAL consortium (n = 43,737) as a replication sample. Results: In ProtecT, the puberty genetic score was inversely associated with prostate cancer grade (odds ratio (OR) of high- vs. low-grade cancer, per tertile of the score: 0.76; 95 \% CI, 0.64-0.89). In an instrumental variable estimation of the causal OR, later physical development in adolescence (equivalent to a difference of one Tanner stage between pubertal boys of the same age) was associated with a 77 \% (95 \% CI, 43-91 \%) reduced odds of high Gleason prostate cancer. In PRACTICAL, the puberty genetic score was associated with prostate cancer stage (OR of advanced vs. localized cancer, per tertile: 0.95; 95 \% CI, 0.91-1.00) and prostate cancer-specific mortality (hazard ratio amongst cases, per tertile: 0.94; 95 \% CI, 0.90-0.98), but not with disease grade. Conclusions: Older age at sexual maturation is causally linked to a reduced risk of later prostate cancer, especially aggressive disease.",

author = "Carolina Bonilla and Lewis, \{Sarah J.\} and Martin, \{Richard M.\} and Donovan, \{Jenny L.\} and Hamdy, \{Freddie C.\} and Neal, \{David E.\} and Rosalind Eeles and Doug Easton and Zsofia Kote-Jarai and \{Al Olama\}, \{Ali Amin\} and \{The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium\} 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 Nora Pashayan 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 Jong Park and Radka Kaneva and Jyotsna Batra and Teixeira, \{Manuel R.\} and Hardev Pandha and Mark Lathrop and Smith, \{George Davey\} and Margaret Cook and Angela Morga 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 Southey, \{Melissa C.\} and Fitzgerald, \{Liesel M.\} and John Pedersen and John Hopper 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 Csilla Sipeky and Roder, \{Martin Andreas\} and Peter Iversen and Peter Klarskov and Nielsen, \{Sune F.\} and Maren Weischer and Key, \{Tim J.\} and Hans Wallinder and Sven Gustafsson and Angela Cox and Anne George and Athene Lane and Gemma Marsden and Michael Davis and Paul Brown and Paul Pharoah and Signorello, \{Lisa B.\} and Wei Zheng and McDonnell, \{Shannon K.\} and Schaid, \{Daniel J.\} and Liang Wang and Lori Tillmans and Shaun Riska and Thomas Schnoeller and Kathleen Herkommer and Manuel Luedeke and Walther Vogel and Dominika Wokozorczyk and Jan Lubiski and Wojciech Kluzniak",

year = "2016",

month = jan,

day = "1",

doi = "10.1186/s12916-016-0602-x",

language = "English",

volume = "14",

pages = "1--11",

journal = "BMC Medicine",

issn = "1741-7015",

publisher = "BioMed Central Ltd.",

number = "1",

}

Bonilla, C, Lewis, SJ, Martin, RM, Donovan, JL, Hamdy, FC, Neal, DE, Eeles, R, Easton, D, Kote-Jarai, Z, Al Olama, AA, The PRACTICAL (Prostate Cancer Association Group to Investigate Cancer-Associated Alterations in the Genome) Consortium & Batra, J 2016, 'Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort', BMC Medicine, vol. 14, no. 1, 66, pp. 1-11. https://doi.org/10.1186/s12916-016-0602-x

TY - JOUR

T1 - Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort

AU - Bonilla, Carolina

AU - Lewis, Sarah J.

AU - Martin, Richard M.

AU - Donovan, Jenny L.

AU - Hamdy, Freddie C.

AU - Neal, David E.

AU - Eeles, Rosalind

AU - Easton, Doug

AU - Kote-Jarai, Zsofia

AU - Al Olama, Ali Amin

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

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 - Pashayan, Nora

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 - Park, Jong

AU - Kaneva, Radka

AU - Batra, Jyotsna

AU - Teixeira, Manuel R.

AU - Pandha, Hardev

AU - Lathrop, Mark

AU - Smith, George Davey

AU - Cook, Margaret

AU - Morga, 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 - Southey, Melissa C.

AU - Fitzgerald, Liesel M.

AU - Pedersen, John

AU - Hopper, John

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 - Sipeky, Csilla

AU - Roder, Martin 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 - Cox, Angela

AU - George, Anne

AU - Lane, Athene

AU - Marsden, Gemma

AU - Davis, Michael

AU - Brown, Paul

AU - Pharoah, Paul

AU - Signorello, Lisa B.

AU - Zheng, Wei

AU - McDonnell, Shannon K.

AU - Schaid, Daniel J.

AU - Wang, Liang

AU - Tillmans, Lori

AU - Riska, Shaun

AU - Schnoeller, Thomas

AU - Herkommer, Kathleen

AU - Luedeke, Manuel

AU - Vogel, Walther

AU - Wokozorczyk, Dominika

AU - Lubiski, Jan

AU - Kluzniak, Wojciech

PY - 2016/1/1

Y1 - 2016/1/1

N2 - Background: Epidemiological studies have observed a positive association between an earlier age at sexual development and prostate cancer, but markers of sexual maturation in boys are imprecise and observational estimates are likely to suffer from a degree of uncontrolled confounding. To obtain causal estimates, we examined the role of pubertal development in prostate cancer using genetic polymorphisms associated with Tanner stage in adolescent boys in a Mendelian randomization (MR) approach. Methods: We derived a weighted genetic risk score for pubertal development, combining 13 SNPs associated with male Tanner stage. A higher score indicated a later puberty onset. We examined the association of this score with prostate cancer risk, stage and grade in the UK-based ProtecT case-control study (n = 2,927), and used the PRACTICAL consortium (n = 43,737) as a replication sample. Results: In ProtecT, the puberty genetic score was inversely associated with prostate cancer grade (odds ratio (OR) of high- vs. low-grade cancer, per tertile of the score: 0.76; 95 % CI, 0.64-0.89). In an instrumental variable estimation of the causal OR, later physical development in adolescence (equivalent to a difference of one Tanner stage between pubertal boys of the same age) was associated with a 77 % (95 % CI, 43-91 %) reduced odds of high Gleason prostate cancer. In PRACTICAL, the puberty genetic score was associated with prostate cancer stage (OR of advanced vs. localized cancer, per tertile: 0.95; 95 % CI, 0.91-1.00) and prostate cancer-specific mortality (hazard ratio amongst cases, per tertile: 0.94; 95 % CI, 0.90-0.98), but not with disease grade. Conclusions: Older age at sexual maturation is causally linked to a reduced risk of later prostate cancer, especially aggressive disease.

AB - Background: Epidemiological studies have observed a positive association between an earlier age at sexual development and prostate cancer, but markers of sexual maturation in boys are imprecise and observational estimates are likely to suffer from a degree of uncontrolled confounding. To obtain causal estimates, we examined the role of pubertal development in prostate cancer using genetic polymorphisms associated with Tanner stage in adolescent boys in a Mendelian randomization (MR) approach. Methods: We derived a weighted genetic risk score for pubertal development, combining 13 SNPs associated with male Tanner stage. A higher score indicated a later puberty onset. We examined the association of this score with prostate cancer risk, stage and grade in the UK-based ProtecT case-control study (n = 2,927), and used the PRACTICAL consortium (n = 43,737) as a replication sample. Results: In ProtecT, the puberty genetic score was inversely associated with prostate cancer grade (odds ratio (OR) of high- vs. low-grade cancer, per tertile of the score: 0.76; 95 % CI, 0.64-0.89). In an instrumental variable estimation of the causal OR, later physical development in adolescence (equivalent to a difference of one Tanner stage between pubertal boys of the same age) was associated with a 77 % (95 % CI, 43-91 %) reduced odds of high Gleason prostate cancer. In PRACTICAL, the puberty genetic score was associated with prostate cancer stage (OR of advanced vs. localized cancer, per tertile: 0.95; 95 % CI, 0.91-1.00) and prostate cancer-specific mortality (hazard ratio amongst cases, per tertile: 0.94; 95 % CI, 0.90-0.98), but not with disease grade. Conclusions: Older age at sexual maturation is causally linked to a reduced risk of later prostate cancer, especially aggressive disease.

UR - https://www.scopus.com/pages/publications/85007425384

U2 - 10.1186/s12916-016-0602-x

DO - 10.1186/s12916-016-0602-x

M3 - Article

C2 - 27044414

AN - SCOPUS:85007425384

SN - 1741-7015

VL - 14

SP - 1

EP - 11

JO - BMC Medicine

JF - BMC Medicine

IS - 1

M1 - 66

ER -

Pubertal development and prostate cancer risk: Mendelian randomization study in a population-based cohort

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