Runs of homozygosity and testicular cancer risk

Loveday, C.; Sud, A.; Litchfield, K.; Levy, M.; Holroyd, A.; Broderick, P.; Kote-Jarai, Z.; Dunning, A. M.; Muir, K.; Peto, J.; Eeles, R.; Easton, D. F.; Dudakia, D.; Orr, N.; Pashayan, N.; Rustin, G.; Srihari, N. N.; Cole, D.; Askill, C.; Bertelli, G.; Barber, J.; Gilby, E.; White, J.; Baybrooke, J.; Leahy, M.; Welch, R.; Chakraborti, P.; Joffe, J.; Brown, R.; Faust, G.; Simmonds, P.; Mazhar, D.; Stockdale, A.; Hrounda, D.; Humber, C.; Appel, W.; Hong, A.; Howard, G.; Douglas, F.; Bloomfield, D.; Butt, M.; Kelly, K.; Mehra, R.; Rogers, P.; Hatton, M.; Hennig, I.; McAteer, J.; Savage, P.; Seckl, M.; Gale, J.; Clark, P.; Woby, S.; Rathmell, A.; Lamont, A.; Sarwar, N.; Stuart, N.; Chowdhury, S.; Beesley, S.; Winkler, M.; Hamid, A.; Pathak, S.; Madhavan, K.; Highley, M.; Money-Kryle, J.; Brock, C.; Sreenivasan, T.; Henderson, B. E.; Haiman, C. A.; Schumacher, F. R.; Al Olama, A. A.; Benlloch, S.; Berndt, S. I.; Conti, D. V.; Wiklund, F.; Chanock, S.; Gapster, S.; Stevens, V. L.; Tangen, C. M.; Batra, J.; Clements, J.; Gronberg, H.; Schleutker, J.; Albanes, D.; Wolk, A.; West, C.; Mucci, L.; Cancel-Tassin, G.; Koutros, S.; Sorensen, K. D.; Maehle, L.; Neal, D. E.; Hamdy, F. C.; Donovan, J. L.; Travis, R. C.; Hamilton, R. J.; Ingles, S. A.; Rosenstein, B. S.; Lu, Y. J.; Giles, G. G.; Kibel, A. S.; Vega Gliemmo, Ana; Kogevinas, M.; Penney, K. L.; Park, J. Y.; Stanford, J. L.; Cybulski, C.; Nordestgaard, B. G.; Brenner, H.; Maier, C.; Kim, J.; John, E. M.; Teixeira, M. R.; Neuhausen, S. L.; Ruyck, K.; Razack, A.; Newcomb, L. F.; Lessel, D.; Kaneva, R.; Usmani, N.; Claessens, F.; Townsend, P. A.; Gago Dominguez, Manuela; Roobol, M. J.; Menegaux, F.; Khaw, K. T.; Cannon-Albrigh, L.; Pandha, H.; Thibodeau, S. N.; Reid, A.; Huddart, R. A.; Houlston, R. S.; Turnbull, C.
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Estatísticas
Estatísticas
Identificadores
Identificadores
URI: http://hdl.handle.net/20.500.11940/15675
PMID: 31310061
ISSN: 2047-2919
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Autor corporativo
UK Testicular Cancer Collaboration; PRACTICAL Consortium
Data de publicación
2019
Título da revista
ANDROLOGY
Tipo de contido
Artigo
DeCS
neoplasias testiculares | homocigoto | genotipo | genoma | factores de riesgo | humanos | estudio de asociación genómica completa | neoplasias
MeSH
Risk Factors | Humans | Genome | Testicular Neoplasms | Genome-Wide Association Study | Genotype | Neoplasms | Homozygote
Resumo
BACKGROUND: Testicular germ cell tumour (TGCT) is highly heritable but > 50% of the genetic risk remains unexplained. Epidemiological observation of greater relative risk to brothers of men with TGCT compared to sons has long alluded to recessively acting TGCT genetic susceptibility factors, but to date none have been reported. Runs of homozygosity (RoH) are a signature indicating underlying recessively acting alleles and have been associated with increased risk of other cancer types. OBJECTIVE: To examine whether RoH are associated with TGCT risk. METHODS: We performed a genome-wide RoH analysis using GWAS data from 3206 TGCT cases and 7422 controls uniformly genotyped using the OncoArray platform. RESULTS: Global measures of homozygosity were not significantly different between cases and controls, and the frequency of individual consensus RoH was not significantly different between cases and controls, after correction for multiple testing. RoH at three regions, 11p13-11p14.3, 5q14.1-5q22.3 and 13q14.11-13q.14.13, were, however, nominally statistically significant at p < 0.01. Intriguingly, RoH200 at 11p13-11p14.3 encompasses Wilms tumour 1 (WT1), a recognized cancer susceptibility gene with roles in sex determination and developmental transcriptional regulation, processes repeatedly implicated in TGCT aetiology. DISCUSSION AND CONCLUSION: Overall, our data do not support a major role in the risk of TGCT for recessively acting alleles acting through homozygosity, as measured by RoH in outbred populations of cases and controls.