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5 research outputs found

The effect on melanoma risk of genes previously associated with telomere length.

Author: Akslen L.A.
AMFS Investigators
Amos C.I.
Andresen P.A.
Avril M.F.
Azizi E.
Barrett J.H.
Bishop D.T.
Bishop J.A.N.
Brossard M.
Brown K.M.
Cust A.E.
Debniak T.
Demenais F.
Doorn R. van
Dunning A.M.
Elder D.E.
Friedman E.
GenoMEL Consortium
Ghiorzo P.
Gillanders E.M.
Goldstein A.M.
Gruis N.A.
Hansson J.
Harland M.
Hayward N.K.
Helsing P.
Hocevar M.
Hoiom V.
IBD Investigators
Iles M.M.
Ingvar C.
Kanetsky P.A.
Landi M.T.
Lang J.
Lathrop G.M.
Law M.H.
Lee J.E.
Lubinski J.
MacGregor S.
Mackie R.M.
Mann G.J.
Martin N.G.
Molven A.
Montgomery G.W.
Moses E.K.
Novakovic S.
Olsson H.
Pharoah P.D.P.
Pooley K.A.
Puig S.
Puig-Butille J.A.
QMEGA Investigator
QTWIN Investigator
Radford-Smith G.L.
Randerson-Moor J.
Scarra G.B.
SDH Study Grp
Stoep N. van der
Taylor J.C.
Ward S.V.
Whiteman D.C.
Publication venue: J Natl Cancer Inst
Publication date: 01/01/2014
Field of study

Telomere length has been associated with risk of many cancers, but results are inconsistent. Seven single nucleotide polymorphisms (SNPs) previously associated with mean leukocyte telomere length were either genotyped or well-imputed in 11108 case patients and 13933 control patients from Europe, Israel, the United States and Australia, four of the seven SNPs reached a P value under .05 (two-sided). A genetic score that predicts telomere length, derived from these seven SNPs, is strongly associated (P = 8.92x10(-9), two-sided) with melanoma risk. This demonstrates that the previously observed association between longer telomere length and increased melanoma risk is not attributable to confounding via shared environmental effects (such as ultraviolet exposure) or reverse causality. We provide the first proof that multiple germline genetic determinants of telomere length influence cancer risk.This is the final version of the article. It first appeared from Oxford University Press via http://dx.doi.org/10.1093/jnci/dju26

University of Bergen

Lund University Publications

Crossref

PubMed Central

Leiden University Scholary Publications

Apollo (Cambridge)

NORA - Norwegian Open Research Archives

Archivio istituzionale della ricerca - Università di Genova

espace@Curtin

University of Melbourne Institutional Repository

Somatic BRAF and NRAS Mutations in Familial Melanomas with Known Germline CDKN2A Status: A GenoMEL Study

Author: Brage S.E.
Doorn R. van
Ghiorzo P.
Gruis N.A.
Hansson J.
Harbst K.
Harland M.
Hayward N.K.
Hoiom V.
Johansson C.H.
Jonsson G.
Kanter-Lewensohn L.
Melanoma Genetics Consortium GenoM
Newton-Bishop J.
Olsson H.
Omholt K.
Palmer J.
Pjanova D.
Puig S.
Scarra G.B.
Vassilaki I.
Zebary A.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2014
Field of study

Dermatology-oncolog

Lund University Publications

Elsevier - Publisher Connector

Leiden University Scholary Publications

Fine mapping of genetic susceptibility loci for melanoma reveals a mixture of single variant and multiple variant regions.

Dermatology-oncolog

Leiden University Scholary Publications

Archivio istituzionale della ricerca - Università di Genova

Overlapping genetic architecture between Parkinson disease and melanoma

Author: 23andMe Research Team
Agee M.
Akslen L.A.
Alipanahi B.
Amos C.I.
Andresen P.A.
Auton A.
Avril M.F.
Azizi E.
Barrett J.H.
Bell R.K.
Benitez B.A.
Bishop D.T.
Bishop J.A.
Brossard M.
Brown K.M.
Bryc K.
Budde J.P.
Burdon K.P.
Chen W.V.
Craig J.E.
Cruchaga C.
Cust A.E.
Davis A.A.
Debniak T.
Demenais F.
Doorn R. van
Dube U.
Duffy D.L.
Dunning A.M.
Easton D.F.
Elder D.E.
Elson S.L.
Fang S.
Fontanillas P.
Friedman E.
Furlotte N.A.
Galan P.
Ghiorzo P.
Gillanders E.M.
Goldstein A.M.
Gruis N.A.
Han J.
Hansson J.
Harari O.
Harland M.
Hayward N.K.
Helsing P.
Hinds D.A.
Hocevar M.
Hoiom V.
Huber K.E.
Ibanez L.
Iles M.M.
Ingvar C.
Kanetsky P.A.
Kleinman A.
Kumar R.
Kypreou K.P.
Landi M.T.
Lang J.
Lathrop G.M.
Law M.H.
Lee J.E.
Litterman N.K.
Lubinski J.
MacGregor S.
Mackie R.M.
Mann G.J.
Martin N.G.
McCreight J.C.
McIntyre M.H.
Melanoma Meta Analysis Consortium
Molven A.
Montgomery G.W.
Moses E.K.
Mountain J.L.
Noblin E.S.
Northover C.A.M.
Novakovic S.
Nyholt D.R.
Olsson H.
Orr N.
Pharoah P.D.
Pitts S.J.
Pooley K.A.
Puig S.
Puig-Butille J.A.
Qureshi A.A.
Radford-Smith G.L.
Randerson-Moor J.
Sathirapongsasuti J.F.
Sazonova O.V.
Scarra G.B.
Schadendorf E.
Schulze H.J.
Shelton J.F.
Shringarpure S.
Simms L.A.
Song F.
Stoep N. van der
Stratigos A.J.
Swerdlow A.J.
Taylor J.C.
Tian C.
Tung J.C.Y.
Vacic V.
Ward S.V.
Whiteman D.C.
Wilson C.H.
Wu W.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/02/2020
Field of study

Epidemiologic studies have reported inconsistent results regarding an association between Parkinson disease (PD) and cutaneous melanoma (melanoma). Identifying shared genetic architecture between these diseases can support epidemiologic findings and identify common risk genes and biological pathways. Here, we apply polygenic, linkage disequilibrium-informed methods to the largest available case-control, genome-wide association study summary statistic data for melanoma and PD. We identify positive and significant genetic correlation (correlation: 0.17, 95% CI 0.10-0.24; P = 4.09 x 10(-06)) between melanoma and PD. We further demonstrate melanoma and PD-inferred gene expression to overlap across tissues (correlation: 0.14, 95% CI 0.06 to 0.22; P = 7.87 x 10(-04)) and highlight seven genes including PIEZO1, TRAPPC2L, and SOX6 as potential mediators of the genetic correlation between melanoma and PD. These findings demonstrate specific, shared genetic architecture between PD and melanoma that manifests at the level of gene expression.Hereditary cancer genetic

Leiden University Scholary Publications

Publisher Correction: Novel pleiotropic risk loci for melanoma and nevus density implicate multiple biological pathways

Author: Akslen L.A.
Amos C.I.
Andresen P.A.
Avril M.F.
Azizi E.
Barrett J.H.
Bataille V.
Beesley J.
Bishop D.T.
Bishop J.A.N.
Bowdler L.
Brossard M.
Brown K.M.
Brown M.A.
Burdon K.P.
Chanock S.
Chen W.V.
Craig J.E.
Cust A.E.
Debniak T.
Demenais F.
Doorn R. van
Duffy D.L.
Dunning A.M.
Easton D.F.
Elder D.E.
Evans D.M.
Falchi M.
Fang S.Y.
Friedman E.
Galan P.
Ghiorzo P.
Gillanders E.M.
Glass D.
Goldstein A.M.
Green A.C.
Gruis N.A.
Han J.
Hansson J.
Harland M.
Hayward N.K.
Heath A.C.
Helsing P.
Henders A.K.
Hewitt A.W.
Hocevar M.
Hoiom V.
Hunter D.J.
Ikram M.A.
Iles M.M.
Ingvar C.
Jacobs L.C.
Kanetsky P.A.
Kayser M.
Kraft P.
Kumar R.
Kypreou K.P.
Landi M.T.
Lang J.
Lathrop G.M.
Law M.H.
Lee J.E.
Li X.
Liu F.
Lubinski J.
MacGregor S.
Mackey D.A.
Mackie R.M.
Madden P.A.
Mann G.J.
Martin N.G.
Melanoma GWAS Consortium
Molven A.
Montgomery G.W.
Moses E.K.
Nelson E.C.
Nijsten T.E.
Novakovic S.
Nyholt D.R.
Olsson H.
Orr N.
Pharoah P.D.P.
Pooley K.A.
Puig S.
Puig-Butille J.A.
Radford-Smith G.L.
Randerson-Moor J.
Sanna M.
Scarra G.B.
Schadendorf D.
Schulze H.J.
Simms L.A.
Smith G.D.
Song F.
Spector T.D.
Stoep N. van der
Stratigos A.J.
Sturm R.A.
Swerdlow A.J.
Taylor J.C.
Uitterlinden A.G.
Visconti A.
Ward S.V.
Whiteman D.C.
Wright M.J.
Yazar S.
Zhu G.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2019
Field of study

Correction to: Nature Communications; https://doi.org/10.1038/s41467-018-06649-5; published online: 14 November 201

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