基因组学为双相情感障碍带来了生物学和表型方面的见解。
Genomics yields biological and phenotypic insights into bipolar disorder.
作者信息
O'Connell Kevin S, Koromina Maria, van der Veen Tracey, Boltz Toni, David Friederike S, Yang Jessica Mei Kay, Lin Keng-Han, Wang Xin, Coleman Jonathan R I, Mitchell Brittany L, McGrouther Caroline C, Rangan Aaditya V, Lind Penelope A, Koch Elise, Harder Arvid, Parker Nadine, Bendl Jaroslav, Adorjan Kristina, Agerbo Esben, Albani Diego, Alemany Silvia, Alliey-Rodriguez Ney, Als Thomas D, Andlauer Till F M, Antoniou Anastasia, Ask Helga, Bass Nicholas, Bauer Michael, Beins Eva C, Bigdeli Tim B, Pedersen Carsten Bøcker, Boks Marco P, Børte Sigrid, Bosch Rosa, Brum Murielle, Brumpton Ben M, Brunkhorst-Kanaan Nathalie, Budde Monika, Bybjerg-Grauholm Jonas, Byerley William, Cabana-Domínguez Judit, Cairns Murray J, Carpiniello Bernardo, Casas Miquel, Cervantes Pablo, Chatzinakos Chris, Chen Hsi-Chung, Clarence Tereza, Clarke Toni-Kim, Claus Isabelle, Coombes Brandon, Corfield Elizabeth C, Cruceanu Cristiana, Cuellar-Barboza Alfredo, Czerski Piotr M, Dafnas Konstantinos, Dale Anders M, Dalkner Nina, Degenhardt Franziska, DePaulo J Raymond, Djurovic Srdjan, Drange Ole Kristian, Escott-Price Valentina, Fanous Ayman H, Fellendorf Frederike T, Ferrier I Nicol, Forty Liz, Frank Josef, Frei Oleksandr, Freimer Nelson B, Fullard John F, Garnham Julie, Gizer Ian R, Gordon Scott D, Gordon-Smith Katherine, Greenwood Tiffany A, Grove Jakob, Guzman-Parra José, Ha Tae Hyon, Hahn Tim, Haraldsson Magnus, Hautzinger Martin, Havdahl Alexandra, Heilbronner Urs, Hellgren Dennis, Herms Stefan, Hickie Ian B, Hoffmann Per, Holmans Peter A, Huang Ming-Chyi, Ikeda Masashi, Jamain Stéphane, Johnson Jessica S, Jonsson Lina, Kalman Janos L, Kamatani Yoichiro, Kennedy James L, Kim Euitae, Kim Jaeyoung, Kittel-Schneider Sarah, Knowles James A, Kogevinas Manolis, Kranz Thorsten M, Krebs Kristi, Kushner Steven A, Lavebratt Catharina, Lawrence Jacob, Leber Markus, Lee Heon-Jeong, Liao Calwing, Lucae Susanne, Lundberg Martin, MacIntyre Donald J, Maier Wolfgang, Maihofer Adam X, Malaspina Dolores, Manchia Mirko, Maratou Eirini, Martinsson Lina, Mattheisen Manuel, McGregor Nathaniel W, McInnis Melvin G, McKay James D, Medeiros Helena, Meyer-Lindenberg Andreas, Millischer Vincent, Morris Derek W, Moutsatsou Paraskevi, Mühleisen Thomas W, O'Donovan Claire, Olsen Catherine M, Panagiotaropoulou Georgia, Papiol Sergi, Pardiñas Antonio F, Park Hye Youn, Perry Amy, Pfennig Andrea, Pisanu Claudia, Potash James B, Quested Digby, Rapaport Mark H, Regeer Eline J, Rice John P, Rivera Margarita, Schulte Eva C, Senner Fanny, Shadrin Alexey, Shilling Paul D, Sigurdsson Engilbert, Sindermann Lisa, Sirignano Lea, Siskind Dan, Slaney Claire, Sloofman Laura G, Smeland Olav B, Smith Daniel J, Sobell Janet L, Soler Artigas Maria, Stein Dan J, Stein Frederike, Su Mei-Hsin, Sung Heejong, Świątkowska Beata, Terao Chikashi, Tesfaye Markos, Tesli Martin, Thorgeirsson Thorgeir E, Thorp Jackson G, Toma Claudio, Tondo Leonardo, Tooney Paul A, Tsai Shih-Jen, Tsermpini Evangelia Eirini, Vawter Marquis P, Vedder Helmut, Vreeker Annabel, Walters James T R, Winsvold Bendik S, Witt Stephanie H, Won Hong-Hee, Ye Robert, Young Allan H, Zandi Peter P, Zillich Lea, Adolfsson Rolf, Alda Martin, Alfredsson Lars, Backlund Lena, Baune Bernhard T, Bellivier Frank, Bengesser Susanne, Berrettini Wade H, Biernacka Joanna M, Boehnke Michael, Børglum Anders D, Breen Gerome, Carr Vaughan J, Catts Stanley, Cichon Sven, Corvin Aiden, Craddock Nicholas, Dannlowski Udo, Dikeos Dimitris, Etain Bruno, Ferentinos Panagiotis, Frye Mark, Fullerton Janice M, Gawlik Micha, Gershon Elliot S, Goes Fernando S, Green Melissa J, Grigoroiu-Serbanescu Maria, Hauser Joanna, Henskens Frans A, Hjerling-Leffler Jens, Hougaard David M, Hveem Kristian, Iwata Nakao, Jones Ian, Jones Lisa A, Kahn René S, Kelsoe John R, Kircher Tilo, Kirov George, Kuo Po-Hsiu, Landén Mikael, Leboyer Marion, Li Qingqin S, Lissowska Jolanta, Lochner Christine, Loughland Carmel, Luykx Jurjen J, Martin Nicholas G, Mathews Carol A, Mayoral Fermin, McElroy Susan L, McIntosh Andrew M, McMahon Francis J, Medland Sarah E, Melle Ingrid, Milani Lili, Mitchell Philip B, Morken Gunnar, Mors Ole, Mortensen Preben Bo, Müller-Myhsok Bertram, Myers Richard M, Myung Woojae, Neale Benjamin M, Nievergelt Caroline M, Nordentoft Merete, Nöthen Markus M, Nurnberger John I, O'Donovan Michael C, Oedegaard Ketil J, Olsson Tomas, Owen Michael J, Paciga Sara A, Pantelis Christos, Pato Carlos N, Pato Michele T, Patrinos George P, Pawlak Joanna M, Ramos-Quiroga Josep Antoni, Reif Andreas, Reininghaus Eva Z, Ribasés Marta, Rietschel Marcella, Ripke Stephan, Rouleau Guy A, Roussos Panos, Saito Takeo, Schall Ulrich, Schalling Martin, Schofield Peter R, Schulze Thomas G, Scott Laura J, Scott Rodney J, Serretti Alessandro, Smoller Jordan W, Squassina Alessio, Stahl Eli A, Stefansson Hreinn, Stefansson Kari, Stordal Eystein, Streit Fabian, Sullivan Patrick F, Turecki Gustavo, Vaaler Arne E, Vieta Eduard, Vincent John B, Waldman Irwin D, Weickert Cynthia S, Weickert Thomas W, Werge Thomas, Whiteman David C, Zwart John-Anker, Edenberg Howard J, McQuillin Andrew, Forstner Andreas J, Mullins Niamh, Di Florio Arianna, Ophoff Roel A, Andreassen Ole A
机构信息
Division of Mental Health and Addiction, Oslo University Hospital, Oslo, Norway.
Center for Precision Psychiatry, University of Oslo, Oslo, Norway.
出版信息
Nature. 2025 Mar;639(8056):968-975. doi: 10.1038/s41586-024-08468-9. Epub 2025 Jan 22.
Bipolar disorder is a leading contributor to the global burden of disease. Despite high heritability (60-80%), the majority of the underlying genetic determinants remain unknown. We analysed data from participants of European, East Asian, African American and Latino ancestries (n = 158,036 cases with bipolar disorder, 2.8 million controls), combining clinical, community and self-reported samples. We identified 298 genome-wide significant loci in the multi-ancestry meta-analysis, a fourfold increase over previous findings, and identified an ancestry-specific association in the East Asian cohort. Integrating results from fine-mapping and other variant-to-gene mapping approaches identified 36 credible genes in the aetiology of bipolar disorder. Genes prioritized through fine-mapping were enriched for ultra-rare damaging missense and protein-truncating variations in cases with bipolar disorder, highlighting convergence of common and rare variant signals. We report differences in the genetic architecture of bipolar disorder depending on the source of patient ascertainment and on bipolar disorder subtype (type I or type II). Several analyses implicate specific cell types in the pathophysiology of bipolar disorder, including GABAergic interneurons and medium spiny neurons. Together, these analyses provide additional insights into the genetic architecture and biological underpinnings of bipolar disorder.
双相情感障碍是全球疾病负担的主要促成因素。尽管遗传度很高(60-80%),但大多数潜在的遗传决定因素仍然未知。我们分析了欧洲、东亚、非裔美国人和拉丁裔血统参与者的数据(158,036例双相情感障碍患者,280万对照),结合了临床、社区和自我报告样本。我们在多血统荟萃分析中确定了298个全基因组显著位点,比之前的发现增加了四倍,并在东亚队列中确定了特定血统的关联。整合精细定位和其他变异到基因定位方法的结果,确定了双相情感障碍病因学中的36个可信基因。通过精细定位优先选择的基因在双相情感障碍患者中富集了超罕见的有害错义和蛋白质截短变异,突出了常见和罕见变异信号的趋同。我们报告了双相情感障碍遗传结构的差异,这取决于患者确诊的来源以及双相情感障碍的亚型(I型或II型)。多项分析表明特定细胞类型参与双相情感障碍的病理生理学,包括GABA能中间神经元和中等棘状神经元。总之,这些分析为双相情感障碍的遗传结构和生物学基础提供了更多见解。
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