Genome-wide association study of over 40,000 bipolar disorder cases provides new insights into the underlying biology

Mullins, Niamh; Aj, Forstner; Ks, O’Connell; Coombes, Brandon J.; Coleman, Jonathan R. I.; Qiao, Zhen; Td, Als; Tb, Bigdeli; Børte, Sigrid; Bryois, Julien; Aw, Charney; Ok, Drange; Mj, Gandal; Hagenaars, SP; Ikeda, Masashi; Kamitaki, Nolan; Kim, Mi‐Hyun; Krebs, Kristi; Παναγιωταροπούλου, Γεωργία; Bm, Schilder; Lg, Sloofman; Steinberg, Stacy; Trubetskoy,; Bs, Winsvold; Won, Hong-Hee; Абрамова, Л. И.; Adorjan, Kristina; Agerbo, Esben; M, Al Eissa; Albani, Diego; Alliey‐Rodriguez, Ney; Anjorin, Adebayo; Antilla,; Antoniou, Anastasia; Awasthi, Swapnil; J, Hyun Baek; Bækvad‐Hansen, Marie; Bass, Nick; Bauer, Michael; Ec, Beins; Se, Bergen; Birner, Armin; C, Bøcker Pedersen; Bøen, Erlend; Mp, Boks; Bosch, Rosa; Brum, Murielle; Bm, Brumpton; Brunkhorst-Kanaan, Nathalie; Budde, Monika; Bybjerg‐Grauholm, Jonas; Byerley, William; Cairns, Murray J.; Casas, Miquel; Cervantes, Pablo; Clarke, Toni‐Kim; Cruceanu, Cristiana; Cuellar‐Barboza, Alfredo; Cunningham, Jonathan W.; Curtis, David; Pm, Czerski; Dale, Anders M.; Dalkner, Nina; Fs, David; Degenhardt, Franziska; Djurovic, Srdjan; Al, Dobbyn; Douzenis, Athanassios; Elvsåshagen, Torbjørn; Escott-Price,; Ferrier, Nicol; Fiorentino, Alessia; Foroud, Tatiana; Forty, Liz; Frank, Josef; Frei, Oleksandr; Nb, Freimer; Frisén, Louise; Gade, Katrin; Garnham, Julie; Gelernter, Joel; M, Marianne Giørtz Pedersen; Ir, Gizer; Sd, Gordon; Gordon‐Smith, Katherine; Ta, Greenwood; Grove, Jakob; Guzmán‐Parra, José; K, Ha; Haraldsson, Magnús; Hautzinger, Martin; Heilbronner, Urs; Hellgren, Dennis; Herms, Stefan; Hoffmann, Per; Pa, Holmans; Huckins, Laura; Jamain, Stéphane; Js, Johnson; Jl, Kalman; Kamatani, Yoichiro; Jl, Kennedy; Kittel‐Schneider, Sarah; Ja, Knowles; Kogevinas, Manolis; Koromina, Maria; Tm, Kranz; Hr, Kranzler; Kubo, Michiaki; Kupka, Ralph; Kushner, Steven A.; Lavebratt, Catharina; Lawrence, Jacob; Leber, Markus; H, Lee; Ph, Lee; Se, Levy; Lewis, Catrin; Liao, Calwing; Lucae, Susanne; Lundberg, Martin; MacIntyre, Donald J.; Maier, Wolfgang; Maihofer, Adam X.; Malaspina, Dolores; Maratou, Eirini; Martinsson, Lina; Mattheisen, Manuel; Nw, McGregor; McGuffin, Peter; McKay, JD; Medeiros, Helena; Se, Medland; Millischer, Vincent; Montgomery, Grant W.; Jl, Moran; Dw, Morris; Tw, Mühleisen; O’Brien, Niamh; O′Donovan, Claire; Loohuis, Olde; Oruč, Lilijana; Papiol, Sergi; Af, Pardiñas; Perry, Amy; Pfennig, Andrea; Porichi, Evgenia; Jb, Potash; Quested, Digby; T, Raj; Mh, Rapaport; Depaulo,; Ej, Regeer; Jp, Rice; Rivas, Fabio; Rivera, Margarita; Roth, Julian; Roussos, Panos; Dm, Ruderfer; Sánchez-Mora, Cristina; Ec, Schulte; Senner, Fanny; Sharp, Sally I.; Pd, Shilling; Sigurðsson, Engilbert; Sirignano, Lea; Slaney, Claire; Ob, Smeland; Jl, Sobell; Hansen, CS; Ms, Artigas; At, Spijker; Dj, Stein; Js, Strauss; B, Beata Świątkowska; Terao, Chikashi; Te, Thorgeirsson; Toma, Claudio; Tooney, Paul A.; Tsermpini, Evangelia‐Eirini; Mp, Vawter; Vedder, Helmut; Jtr, Walters; Witt, Stephanie H.; Shi, Xi; Xu, Wentao; Young, Hannah; Ah, Young; Pp, Zandi; Zhou, Hang; Zillich, Lea; Adolfsson, Rolf; Agartz, Ingrid; Alda, Martin; Alfredsson, Lars; Babadjanova, Gulja; Backlund, Lena; Bt, Baune; Bellivier, Frank; Bengesser, Susanne; Wh, Berrettini; Dhr., Blackwood; Boehnke, Michael; Børglum, Anders D.; Breen, Gerome; Carr, Vaughan J.; Catts, Stanley V.; Corvin, Aiden; Craddock, Nicholas; Dannlowski, Udo; Dikeos, Dimitris; Esko, Tõnu; Étain, Bruno; Ferentinos, Panagiotis; Frye, Mark A.; Jm, Fullerton; Gawlik, Micha; Es, Gershon; Goes, Fernando S.; Mj, Green; Grigoroiu‐Serbanescu, Maria; Hauser, Joanna; Henskens, Frans; Hillert, Jan; Ks, Hong; Dm, Hougaard; Cm, Hultman; Hveem, Kristian; Iwata, Nakao; Av, Jablensky; Jones, Ian; La, Jones; Kahn, R.S.; Kelsoe,; Kirov, George; M, Mikael Landén; Marion,

doi:10.1101/2020.09.17.20187054

Cited by 34 publications

(60 citation statements)

References 137 publications

(189 reference statements)

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“…Further PTV enrichment was observed in the top 50 genes over the FDR < 5% set; OR = 2.02, P = 8.14 × 10 −7 , but this significant enrichment was not observed as we moved down through the genes displaying ultra-rare damaging case-control enrichment in SCHEMA (genes 51-100; OR = 0.936, P = 0.680, genes 101-150; OR = 1.03, P = 0.794, genes 151-200; OR = 1.07, P = 0.686). We also did not observe PTV enrichment of ultra-rare damaging variation in the recently fine-mapped schizophrenia genes published by the PGC ( 11 ): OR = 1.10, P = 0.178.…”

Section: Resultscontrasting

confidence: 52%

“…To date, GWAS meta-analysis of common SNPs have now identified 64 independent loci that contribute to BD susceptibility, implicating genes encoding ion channels, neurotransmitter transporters, and synaptic and calcium signalling pathways ( 3, 11 ). Evidence of rare variation on BD risk, however, remains inconclusive as sample sizes are substantially smaller than GWAS.…”

Section: Introductionmentioning

confidence: 99%

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Exome sequencing in bipolar disorder reveals shared risk geneAKAP11with schizophrenia

Palmer

Howrigan

Chapman

et al. 2021

Preprint

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Here we report results from the Bipolar Exome (BipEx) collaboration analysis of whole exome sequencing of 13,933 individuals diagnosed with bipolar disorder (BD), matched with 14,422 controls. We find an excess of ultra-rare protein-truncating variants (PTVs) in BD patients among genes under strong evolutionary constraint, a signal evident in both major BD subtypes, bipolar 1 disorder (BD1) and bipolar 2 disorder (BD2). We also find an excess of ultra-rare PTVs within genes implicated from a recent schizophrenia exome meta-analysis (SCHEMA; 24,248 SCZ cases and 97,322 controls) and among binding targets of CHD8. Genes implicated from GWAS of BD, however, are not significantly enriched for ultra-rare PTVs. Combining BD gene-level results with SCHEMA, AKAP11 emerges as a definitive risk gene (ultra-rare PTVs seen in 33 cases and 13 controls, OR = 7.06, P = 2.83 × 10-9). At the protein level, AKAP-11 is known to interact with GSK3B, the hypothesized mechanism of action for lithium, one of the few treatments for BD. Overall, our results lend further support to the polygenic basis of BD and demonstrate a role for rare coding variation as a significant risk factor in BD onset.

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Section: Resultscontrasting

confidence: 52%

Section: Introductionmentioning

confidence: 99%

Exome sequencing in bipolar disorder reveals shared risk geneAKAP11with schizophrenia

Palmer

Howrigan

Chapman

et al. 2021

Preprint

Self Cite

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“…For example, they include four calcium channels ( CACNA1C, CACNA2D4, CACNB2 , and CACNG8 ), three glutamate receptors (GRIK2, GRIN2A , and GRM8 ), four GABA receptors ( GABRA5, GABRG3, GABRG3 , and GABRP ), and nine potassium channels ( KCNA1, KCNA4, KCNA7, KCNAB2, KCNAB2, KCND3, KCND3, KCNE1 , and KCNG2 ). A recent GWAS showed enrichment of GWAS signals in calcium signaling genes and genes expressed in neurons 69 . The current finding of DNA methylation changes in ion channels, including calcium channels, sheds light on the potential roles of these channels in nonneurons, such as oligodendrocytes, microglia, and astrocytes, in BD.…”

Section: Discussionmentioning

confidence: 99%

Decreased DNA methylation at promoters and gene-specific neuronal hypermethylation in the prefrontal cortex of patients with bipolar disorder

Bundo

Ueda

Nakachi

et al. 2020

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Bipolar disorder (BD) is a severe mental disorder characterized by repeated mood swings. Although genetic factors are collectively associated with the etiology of BD, the underlying molecular mechanisms, particularly how environmental factors affect the brain, remain largely unknown. We performed promoter-wide DNA methylation analysis of neuronal and nonneuronal nuclei in the prefrontal cortex of patients with BD (N=34) and controls (N=35). We found decreased DNA methylation at promoters in both cell types in the BD patients compared to the controls. Gene Ontology (GO) analysis of differentially methylated region (DMR)-associated genes revealed enrichment of molecular motor-related genes in neurons, chemokines in both cell types, and ion channel- and transporter-related genes in nonneurons. Detailed analysis further revealed that growth cone- and dendrite-related genes, including NTRK2 and GRIN1, were hypermethylated in neurons of BD patients. To assess the effect of medication, neuroblastoma cells were cultured under therapeutic concentrations of three different mood stabilizers (lithium, valproate, and carbamazepine). We observed that up to 37.9% of DMRs detected in BD overlapped with mood stabilizer-induced DMRs. Interestingly, mood stabilizer-induced DMRs showed the opposite direction of changes in DMRs in BD, suggesting the therapeutic effects of mood stabilizers on DNA methylation. Among the DMRs, 12 overlapped with loci identified by a previous genome-wide association study of BD. Finally, we performed qPCR analysis of 10 DNA methylation-related genes and found that DNMT3B was overexpressed in BD. The cell type-specific DMRs identified in this study will be useful for understanding the pathophysiology of BD.

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“…As such, the polygenic score may (in part) be capturing variability in cell-extracellular matrix adhesion. Cell-extracellular matrix adhesion is fundamental to cell crawling and axon guidance [41][42][43] , which has also been implicated in psychiatric disorders 15,[19][20][21] . The composition of the extracellular matrix, and increased adhesion of cells to the matrix, has been shown to increase neurite extension in neurons 42,43 , to stimulate gyrification in the developing human neocortex 44 , and to promote branching and migration of neurons 42,45 , among other roles 42 .…”

Section: Discussionmentioning

confidence: 99%

“…It also is feasible that the polygenic components studied may affect the morphology of iPSCs directly. For example, genes involved in neuronal morphology have been implicated in numerous GWAS of psychiatric disorders 15,[19][20][21] . While strongest in neurons, these effects may also be apparent in the morphology of cells more generally, particularly in iPSCs, whose cellular fate is undetermined.…”

Section: Introductionmentioning

confidence: 99%

Feasibility and application of polygenic score analysis to the morphology of human induced pluripotent stem cells

Coleman

2020

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Genome-wide association studies have identified thousands of significant associations between genetic variants and complex traits. Inferring biological insights from these associations has been challenging. One approach attempted has been to examine the effects of individual variants in cellular models. Here, I demonstrate the feasibility of examining the aggregate effect of many variants on cellular phenotypes. I examine the effects of polygenic scores for cross-psychiatric disorder risk, schizophrenia, body mass index and height on cellular morphology, using 1.5 million induced pluripotent stem cells (iPSC) from 60 European-ancestry donors from the Human iPSC Initiative dataset. I show that measuring multiple cells per donor provides sufficient power for polygenic score analyses, and that cross-psychiatric disorder risk is associated with cell area (p = 0.004). Combined with emerging methods of high-throughput iPSC phenotyping, cellular polygenic scoring is a promising method for understanding potential biological effects of the polygenic component of complex traits.

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Genome-wide association study of over 40,000 bipolar disorder cases provides new insights into the underlying biology

Cited by 34 publications

References 137 publications

Exome sequencing in bipolar disorder reveals shared risk geneAKAP11with schizophrenia

Exome sequencing in bipolar disorder reveals shared risk geneAKAP11with schizophrenia

Decreased DNA methylation at promoters and gene-specific neuronal hypermethylation in the prefrontal cortex of patients with bipolar disorder

Feasibility and application of polygenic score analysis to the morphology of human induced pluripotent stem cells

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