Abstract

Schizophrenia (SZ) and bipolar disorder (BP) are the most chronic and debilitating of psychiatric syndromes, each with lifetime prevalence of about 1%. Existing pharmacologic treatments are partially effective in reducing symptom severity but do not ameliorate the underlying disease processes, cognitive deficits, or functional disabilities associated with these syndromes. Given that both SZ and BP are substantially heritable, gene discovery represents our best hope for identifying new molecular targets for interventions. However, the highly polygenic and heterogeneous nature of these syndromes substantially reduces the effectiveness of traditional genetic linkage and association designs. In addition, recent evidence suggests that some genetic overlaps between these conditions. Our approach is based on the premise that SZ and BP are best conceptualized as sets of quantitative traits that reflect intermediate phenotypes between predisposing genes and syndromal expression (CEendophenotypes1). Here we will screen 300,000 SNP markers - distributed so as to enable the detection of linkage disequilibrium in most parts of the genome - for association with memory and sociability phenotypes previously associated with risk for SZ and BP in a sample of 2,000 subjects from the greater Los Angeles area (LA2K sample). Followup studies of patients with SZ and BP will be performed to specify the impact of the genes identified in the LA2K sample on neuroanatomical and neurophysiological indicators of the pathophysiology of SZ and BP. Because nearly half of the genome is expressed in the brain, and considering the central importance of memory and sociability to adaptive behavioral function, there are likely dozens to hundreds of genes of small to moderate effect influencing these phenotypes in the general population. We hypothesize that many of these genes contribute to susceptibility to SZ and BP through their impacts on the brain systems mediating memory systems and social function and that most of these have been undetected by previous studies using syndromal status as the phenotypic target. In parallel with this whole genome strategy, and to illustrate our translational approach, we will use rodent transgenic models of two promising candidate genes DISC1 and Dysbindin to specify the cellular mechanisms underlying the associations of these genes with memory, sociabiliy, and susceptibility to SZ and BP.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Linked Research project Grant (RL1)
Project #
5RL1MH083269-05
Application #
8091406
Study Section
Special Emphasis Panel (ZRR1-SRC (99))
Program Officer
Rumsey, Judith M
Project Start
2007-09-29
Project End
2012-06-30
Budget Start
2011-07-01
Budget End
2012-06-30
Support Year
5
Fiscal Year
2011
Total Cost
$209,949
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Orban, Pierre; Dansereau, Christian; Desbois, Laurence et al. (2018) Multisite generalizability of schizophrenia diagnosis classification based on functional brain connectivity. Schizophr Res 192:167-171
Trampush, J W; Yang, M L Z; Yu, J et al. (2017) GWAS meta-analysis reveals novel loci and genetic correlates for general cognitive function: a report from the COGENT consortium. Mol Psychiatry 22:336-345
Lam, Max; Trampush, Joey W; Yu, Jin et al. (2017) Large-Scale Cognitive GWAS Meta-Analysis Reveals Tissue-Specific Neural Expression and Potential Nootropic Drug Targets. Cell Rep 21:2597-2613
Poldrack, R A; Congdon, E; Triplett, W et al. (2016) A phenome-wide examination of neural and cognitive function. Sci Data 3:160110
Spiegel, S; Chiu, A; James, A S et al. (2015) Recognition deficits in mice carrying mutations of genes encoding BLOC-1 subunits pallidin or dysbindin. Genes Brain Behav 14:618-24
Robertson, Chelsea L; Ishibashi, Kenji; Mandelkern, Mark A et al. (2015) Striatal D1- and D2-type dopamine receptors are linked to motor response inhibition in human subjects. J Neurosci 35:5990-7
Haut, Kristen M; Karlsgodt, Katherine H; Bilder, Robert M et al. (2015) Memory systems in schizophrenia: Modularity is preserved but deficits are generalized. Schizophr Res 168:223-30
White, Corey N; Congdon, Eliza; Mumford, Jeanette A et al. (2014) Decomposing decision components in the stop-signal task: a model-based approach to individual differences in inhibitory control. J Cogn Neurosci 26:1601-14
Congdon, Eliza; Altshuler, Lori L; Mumford, Jeanette A et al. (2014) Neural activation during response inhibition in adult attention-deficit/hyperactivity disorder: preliminary findings on the effects of medication and symptom severity. Psychiatry Res 222:17-28
Thakkar, Katharine N; Congdon, Eliza; Poldrack, Russell A et al. (2014) Women are more sensitive than men to prior trial events on the Stop-signal task. Br J Psychol 105:254-72

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