Abstract

Project 3: Role of a psychiatric disease risk factor in synaptic function and gene transcription regulation ABSTRACT Genetic complexity underlying the vast majority of mental disorders has made the study of these diseases exceptionally challenging. Many risk-associated genes have been identified but the biological role is largely unknown. Dysregulated neurodevelopment with altered structural and functional connectivity is believed to underlie many neuropsychiatric disorders and ?a disease of synapses? is the major hypothesis for the biological basis of schizophrenia and other major psychiatric disorders. However, little is known about pathophysiology of synapses in patient neurons, underlying molecular and cellular mechanisms, and to what extent psychiatric disorders may share these mechanisms. Disrupted in Schizophrenia 1 (DISC1) is a gene in which mutations have been associated with increased risk for schizophrenia, bipolar disorder, and other major psychiatric disorders. A large number of animal studies have shown that DISC1 affects multiple neurodevelopmental processes, including synapse formation. Understanding synaptic dysfunction in major psychiatric disease requires direct investigation of synapse properties in human neurons derived from patients with these disorders. Reprogramming patient somatic cells enables recapitulation of normal and pathological human tissue developmental properties in defined conditions and a new way to identify the cellular processes underlying complex human diseases, which can lead to mechanism-based drug discovery. A rare mutation of a 4 base-pair frame-shift deletion at the C-terminus of DISC1 was discovered to co-segregate with major psychiatric disorders in a smaller American family (Pedigree H). The current project is built upon our initial results showing that forebrain neurons derived from iPSCs with the DISC1 mutation exhibit significant synaptic defects and RNA-seq analysis showed significant dysregulation of a large number of neuronal genes related to synaptic function and psychiatric disorders in patient neurons. Recent studies using iPSCs from idiopathic schizophrenia patients also showed similar defects in synaptic function and share multiple dysregulated genes. Project 3 will test the hypothesis that a psychiatric disorder risk gene modulates synaptic function of human neurons via biochemical and transcriptional dysregulation, a core defect that may also be present in idiopathic schizophrenia and bipolar patient-derived neurons.
Aim 1 will characterize cellular phenotypes of human cortical neurons differentiated from Pedigree H and idiopathic schizophrenia patient iPSCs.
Aim 2 will determine the role of mutant DISC1 in iPSC-derived astrocytes.
Aim 3 will evaluate neuronal subtype specificity of mutant DISC1 effects on neuronal development, synaptic function and transcription.
Each aim requires the involvement of at least one academic and one industrial partner as well as Core B at Janssen and is designed to incorporate cross-validation across labs and establish protocols that can be disseminated for further validation. Cellular phenotypes will be compared to other iPSC lines in the NCRCRG and will be further developed into miniaturized assays via Core C at SBMRI for future drug screens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Program--Cooperative Agreements (U19)
Project #
1U19MH106434-01A1
Application #
8999335
Study Section
Special Emphasis Panel (ZMH1-ERB-C (06))
Project Start
Project End
Budget Start
2015-09-01
Budget End
2016-08-31
Support Year
1
Fiscal Year
2016
Total Cost
$678,080
Indirect Cost
$262,080

  Institution

Name
Johns Hopkins University
Department
Type
DUNS #
001910777
City
Baltimore
State
MD
Country
United States
Zip Code
21205

  Publications

Mansour, Abed AlFatah; Gonçalves, J Tiago; Bloyd, Cooper W et al. (2018) An in vivo model of functional and vascularized human brain organoids. Nat Biotechnol 36:432-441
Sarkar, Anindita; Mei, Arianna; Paquola, Apua C M et al. (2018) Efficient Generation of CA3 Neurons from Human Pluripotent Stem Cells Enables Modeling of Hippocampal Connectivity In Vitro. Cell Stem Cell 22:684-697.e9
Yoon, Ki-Jun; Vissers, Caroline; Ming, Guo-Li et al. (2018) Epigenetics and epitranscriptomics in temporal patterning of cortical neural progenitor competence. J Cell Biol 217:1901-1914
Stern, S; Santos, R; Marchetto, M C et al. (2018) Neurons derived from patients with bipolar disorder divide into intrinsically different sub-populations of neurons, predicting the patients' responsiveness to lithium. Mol Psychiatry 23:1453-1465
Qian, Xuyu; Jacob, Fadi; Song, Mingxi Max et al. (2018) Generation of human brain region-specific organoids using a miniaturized spinning bioreactor. Nat Protoc 13:565-580
McInnis, Melvin G; Assari, Shervin; Kamali, Masoud et al. (2018) Cohort Profile: The Heinz C. Prechter Longitudinal Study of Bipolar Disorder. Int J Epidemiol 47:28-28n
Vadodaria, Krishna C; Stern, Shani; Marchetto, Maria C et al. (2018) Serotonin in psychiatry: in vitro disease modeling using patient-derived neurons. Cell Tissue Res 371:161-170
Vadodaria, Krishna C; Amatya, Debha N; Marchetto, Maria C et al. (2018) Modeling psychiatric disorders using patient stem cell-derived neurons: a way forward. Genome Med 10:1
Ye, Fei; Kang, Eunchai; Yu, Chuan et al. (2017) DISC1 Regulates Neurogenesis via Modulating Kinetochore Attachment of Ndel1/Nde1 during Mitosis. Neuron 96:1041-1054.e5
Yoon, Ki-Jun; Song, Guang; Qian, Xuyu et al. (2017) Zika-Virus-Encoded NS2A Disrupts Mammalian Cortical Neurogenesis by Degrading Adherens Junction Proteins. Cell Stem Cell 21:349-358.e6

Showing the most recent 10 out of 21 publications