Large-scale genomic analyses link reproductive aging to hypothalamic signaling, breast cancer susceptibility and BRCA1-mediated DNA repair

大规模基因组分析将生殖衰老与下丘脑信号传导、乳腺癌易感性和BRCA1介导的DNA修复联系起来。

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作者：Day,Felix R,Ruth,Katherine S,Thompson,Deborah J,Lunetta,Kathryn L,Pervjakova,Natalia,Chasman,Daniel I,Stolk,Lisette,Finucane,Hilary K,Sulem,Patrick,Bulik-Sullivan,Brendan,Esko,Tõnu,Johnson,Andrew D,Elks,Cathy E,Franceschini,Nora,He,Chunyan,Altmaier,Elisabeth,Brody,Jennifer A,Franke,Lude L,Huffman,Jennifer E,Keller,Margaux F,McArdle,Patrick F,Nutile,Teresa,Porcu,Eleonora,Robino,Antonietta,Rose,Lynda M,Schick,Ursula M,Smith,Jennifer A,Teumer,Alexander,Traglia,Michela,Vuckovic,Dragana,Yao,Jie,Zhao,Wei,Albrecht,Eva,Amin,Najaf,Corre,Tanguy,Hottenga,Jouke-Jan,Mangino,Massimo,Smith,Albert V,Tanaka,Toshiko,Abecasis,Goncalo,Andrulis,Irene L,Anton-Culver,Hoda,Antoniou,Antonis C,Arndt,Volker,Arnold,Alice M,Barbieri,Caterina,Beckmann,Matthias W,Beeghly-Fadiel,Alicia,Benitez,Javier,Bernstein,Leslie,Bielinski,Suzette J,Blomqvist,Carl,Boerwinkle,Eric,Bogdanova,Natalia V,Bojesen,Stig E,Bolla,Manjeet K,Borresen-Dale,Anne-Lise,Boutin,Thibaud S,Brauch,Hiltrud,Brenner,Hermann,Brüning,Thomas,Burwinkel,Barbara,Campbell,Archie,Campbell,Harry,Chanock,Stephen J,Chapman,J Ross,Chen,Yii-Der Ida,Chenevix-Trench,Georgia,Couch,Fergus J,Coviello,Andrea D,Cox,Angela,Czene,Kamila,Darabi,Hatef,De Vivo,Immaculata,Demerath,Ellen W,Dennis,Joe,Devilee,Peter,Dörk,Thilo,Dos-Santos-Silva,Isabel,Dunning,Alison M,Eicher,John D,Fasching,Peter A,Faul,Jessica D,Figueroa,Jonine,Flesch-Janys,Dieter,Gandin,Ilaria,Garcia,Melissa E,García-Closas,Montserrat,Giles,Graham G,Girotto,Giorgia G,Goldberg,Mark S,González-Neira,Anna,Goodarzi,Mark O,Grove,Megan L,Gudbjartsson,Daniel F,Guénel,Pascal,Guo,Xiuqing,Haiman,Christopher A,Hall,Per,Hamann,Ute,Henderson,Brian E,Hocking,Lynne J,Hofman,Albert,Homuth,Georg,Hooning,Maartje J,Hopper,John L,Hu,Frank B,Huang,Jinyan,Humphreys,Keith,Hunter,David J,Jakubowska,Anna,Jones,Samuel E,Kabisch,Maria,Karasik,David,Knight,Julia A,Kolcic,Ivana,Kooperberg,Charles,Kosma,Veli-Matti,Kriebel,Jennifer,Kristensen,Vessela,Lambrechts,Diether,Langenberg,Claudia,Li,Jingmei,Li,Xin,Lindström,Sara,Liu,Yongmei,Luan,Jian'an,Lubinski,Jan,Mägi,Reedik,Mannermaa,Arto,Manz,Judith,Margolin,Sara,Marten,Jonathan,Martin,Nicholas G,Masciullo,Corrado,Meindl,Alfons,Michailidou,Kyriaki,Mihailov,Evelin,Milani,Lili,Milne,Roger L,Müller-Nurasyid,Martina,Nalls,Michael,Neale,Ben M,Nevanlinna,Heli,Neven,Patrick,Newman,Anne B,Nordestgaard,Børge G,Olson,Janet E,Padmanabhan,Sandosh,Peterlongo,Paolo,Peters,Ulrike,Petersmann,Astrid,Peto,Julian,Pharoah,Paul D P,Pirastu,Nicola N,Pirie,Ailith,Pistis,Giorgio,Polasek,Ozren,Porteous,David,Psaty,Bruce M,Pylkäs,Katri,Radice,Paolo,Raffel,Leslie J,Rivadeneira,Fernando,Rudan,Igor,Rudolph,Anja,Ruggiero,Daniela,Sala,Cinzia F,Sanna,Serena,Sawyer,Elinor J,Schlessinger,David,Schmidt,Marjanka K,Schmidt,Frank,Schmutzler,Rita K,Schoemaker,Minouk J,Scott,Robert A,Seynaeve,Caroline M,Simard,Jacques,Sorice,Rossella,Southey,Melissa C,Stöckl,Doris,Strauch,Konstantin,Swerdlow,Anthony,Taylor,Kent D,Thorsteinsdottir,Unnur,Toland,Amanda E,Tomlinson,Ian,Truong,Thérèse,Tryggvadottir,Laufey,Turner,Stephen T,Vozzi,Diego,Wang,Qin,Wellons,Melissa,Willemsen,Gonneke,Wilson,James F,Winqvist,Robert,Wolffenbuttel,Bruce B H R,Wright,Alan F,Yannoukakos,Drakoulis,Zemunik,Tatijana,Zheng,Wei,Zygmunt,Marek,Bergmann,Sven,Boomsma,Dorret I,Buring,Julie E,Ferrucci,Luigi,Montgomery,Grant W,Gudnason,Vilmundur,Spector,Tim D,van Duijn,Cornelia M,Alizadeh,Behrooz Z,Ciullo,Marina,Crisponi,Laura,Easton,Douglas F,Gasparini,Paolo P,Gieger,Christian,Harris,Tamara B,Hayward,Caroline,Kardia,Sharon L R,Kraft,Peter,McKnight,Barbara,Metspalu,Andres,Morrison,Alanna C,Reiner,Alex P,Ridker,Paul M,Rotter,Jerome I,Toniolo,Daniela,Uitterlinden,André G,Ulivi,Sheila,Völzke,Henry,Wareham,Nicholas J,Weir,David R,Yerges-Armstrong,Laura M,Price,Alkes L,Stefansson,Kari,Visser,Jenny A,Ong,Ken K,Chang-Claude,Jenny,Murabito,Joanne M,Perry,John R B,Murray,Anna

期刊：	Nature Genetics	影响因子：	29.000
时间：	2015	起止号：	2015 Nov;47(11):1294-1303
doi：	10.1038/ng.3412	靶点：	BRCA1
研究方向：	肿瘤、信号转导、神经科学、免疫/内分泌	疾病类型：	乳腺癌、衰老

Abstract

Menopause timing has a substantial impact on infertility and risk of disease, including breast cancer, but the underlying mechanisms are poorly understood. We report a dual strategy in ∼70,000 women to identify common and low-frequency protein-coding variation associated with age at natural menopause (ANM). We identified 44 regions with common variants, including two regions harboring additional rare missense alleles of large effect. We found enrichment of signals in or near genes involved in delayed puberty, highlighting the first molecular links between the onset and end of reproductive lifespan. Pathway analyses identified major association with DNA damage response (DDR) genes, including the first common coding variant in BRCA1 associated with any complex trait. Mendelian randomization analyses supported a causal effect of later ANM on breast cancer risk (∼6% increase in risk per year; P = 3 × 10(-14)), likely mediated by prolonged sex hormone exposure rather than DDR mechanisms.

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