Activity-Dependent Changes in Gene Expression in Schizophrenia Human-Induced Pluripotent Stem Cell Neurons

Roussos, Panos; Guennewig, Boris; Kaczorowski, Dominik C.; Barry, Guy; Brennand, Kristen J.

doi:10.1001/jamapsychiatry.2016.2575

Cited by 39 publications

(37 citation statements)

References 34 publications

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“…596 genes were differentially expressed in neurons derived from schizophrenic patients versus controls, reflecting the phenotypic differences between the differentiated neuronal populations (Brennand et al, 2011). Previous work has shown that schizophrenia hiPSC-derived NPCs have aberrant migration (Brennand et al, 2014b) and cellular polarity (Yoon et al, 2014), perturbed WNT signaling (Srikanth et al, 2015; Topol et al, 2015b), increased oxidative stress (Brennand et al, 2014b; Paulsen et al, 2011; Robicsek et al, 2013) and altered responses to environmental stressors (Hashimoto-Torii et al, 2014); while schizophrenia hiPSC-derived neurons exhibit decreased neurite number (Brennand et al, 2011), reduced synaptic maturation (Brennand et al, 2011; Robicsek et al, 2013; Wen et al, 2014; Yu et al, 2014) and synaptic activity (Wen et al, 2014; Yu et al, 2014), and blunted activity-dependent response (Roussos et al, 2016). Extensive immunocytochemical validation of the NPC lines used in the present study showed they are positive for diverse NPC markers including nestin, Sox2, vimentin, Pax6 and TBR2(Brennand et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Common developmental genome deprogramming in schizophrenia — Role of Integrative Nuclear FGFR1 Signaling (INFS)

Narla

Lee

et al. 2017

Schizophrenia Research

109

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The watershed-hypothesis of schizophrenia asserts that over 200 different mutations dysregulate distinct pathways that converge on an unspecified common mechanism(s) that controls disease ontogeny. Consistent with this hypothesis, our RNA-sequencing of neuron committed cells (NCCs) differentiated from established iPSCs of 4 schizophrenia patients and 4 control subjects uncovered a dysregulated transcriptome of 1349 mRNAs common to all patients. Data reveal global dysregulation of developmental genome, deconstruction of coordinated mRNA, and mRNA networks, and the formation of aberrant, new coordinated mRNA networks indicating a concerted action of the responsible factor(s). Sequencing of miRNA transcriptomes demonstrated an overexpression of 16 miRNAs and deconstruction of coordinated miRNA–mRNA networks in schizophrenia NCCs. ChiPseq revealed that the nuclear (n) form of FGFR1, a pan-ontogenic regulator, is overexpressed in schizophrenia NCCs and overtargets dysregulated mRNA and miRNA genes. The nFGFR1 targeted 54% of all human gene promoters and 84.4% of schizophrenia dysregulated genes. The upregulated genes reside within major developmental pathways that control neurogenesis and neuron formation, whereas downregulated genes are involved in oligodendrogenesis. Our results indicate (i) an early (preneuronal) genomic etiology of schizophrenia, (ii) dysregulated genes and new coordinated gene networks are common to unrelated cases of schizophrenia, (iii) gene dysregulations are accompanied by increased nFGFR1-genome interactions, and (iv) modeling of increased nFGFR1 by an overexpression of a nFGFR1 lead to up or downregulation of selected genes as observed in schizophrenia NCCs. Together our results designate nFGFR1 signaling as a potential common dysregulated mechanism in investigated patients and potential therapeutic target in schizophrenia.

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Section: Introductionmentioning

confidence: 99%

Common developmental genome deprogramming in schizophrenia — Role of Integrative Nuclear FGFR1 Signaling (INFS)

Narla

Lee

et al. 2017

Schizophrenia Research

109

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“…In light of the retained spontaneous activity in SCZ iPSC-neurons, Roussos et al [ 76 ] moved on to investigate differences in activity dependent gene expression. Potassium chloride treatment was used for neuronal depolarization of iPSC-derived case/control forebrain neurons.…”

Section: Introductionmentioning

confidence: 99%

Tracing Early Neurodevelopment in Schizophrenia with Induced Pluripotent Stem Cells

Ahmad

Sportelli

Ziller

et al. 2018

Cells

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Schizophrenia (SCZ) is a devastating mental disorder that is characterized by distortions in thinking, perception, emotion, language, sense of self, and behavior. Epidemiological evidence suggests that subtle perturbations in early neurodevelopment increase later susceptibility for disease, which typically manifests in adolescence to early adulthood. Early perturbations are thought to be significantly mediated through incompletely understood genetic risk factors. The advent of induced pluripotent stem cell (iPSC) technology allows for the in vitro analysis of disease-relevant neuronal cell types from the early stages of human brain development. Since iPSCs capture each donor’s genotype, comparison between neuronal cells derived from healthy and diseased individuals can provide important insights into the molecular and cellular basis of SCZ. In this review, we discuss results from an increasing number of iPSC-based SCZ/control studies that highlight alterations in neuronal differentiation, maturation, and neurotransmission in addition to perturbed mitochondrial function and micro-RNA expression. In light of this remarkable progress, we consider also ongoing challenges from the field of iPSC-based disease modeling that call for further improvements on the generation and design of patient-specific iPSC studies to ultimately progress from basic studies on SCZ to tailored treatments.

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“…WGCNA ( 13 , 64 ) uses gene-gene Pearson’s correlation indices as a continuous, i.e., weighted, measure of gene-gene relationships. We computed unsigned networks, i.e., negatively correlated genes are considered connected rather than non-connected ( 65 ). The correlation matrix was transformed into an adjacency matrix by raising Pearson’s coefficients to a positive exponent, β, which is chosen to meet the “scale-free” power law connectivity distribution.…”

Section: Methodsmentioning

confidence: 99%

Prefrontal co-expression of schizophrenia risk genes is associated with treatment response in patients

Pergola

Carlo

Jaffe

et al. 2018

Preprint

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Gene co-expression networks are relevant to functional and clinical translation of schizophrenia (SCZ) risk genes. We hypothesized that SCZ risk genes may converge into coexpression pathways which may be associated with gene regulation mechanisms and with response to treatment in patients with SCZ. We identified gene co-expression networks in two prefrontal cortex post-mortem RNA sequencing datasets (total N=688) and replicated them in four more datasets (total N=227). We identified and replicated (all p-values<.001) a single module enriched for SCZ risk loci (13 risk genes in 10 loci). In silico screening of potential regulators of the SCZ risk module via bioinformatic analyses identified two transcription factors and three miRNAs associated with the risk module. To translate post-mortem information into clinical phenotypes, we identified polymorphisms predicting co-expression and combined them to obtain an index approximating module co-expression (Polygenic Co-expression Index: PCI). The PCI-co-expression association was successfully replicated in two independent brain transcriptome datasets (total N=131; all p-values<.05). Finally, we tested the association between the PCI and short-term treatment response in two independent samples of patients with SCZ treated with olanzapine (total N=167). The PCI was associated with treatment response in the positive symptom domain in both clinical cohorts (all p-values<.05).In summary, our findings in a large sample of human post-mortem prefrontal cortex show that coexpression of a set of genes enriched for schizophrenia risk genes is relevant to treatment response. This co-expression pathway may be co-regulated by transcription factors and miRNA associated with it.

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Activity-Dependent Changes in Gene Expression in Schizophrenia Human-Induced Pluripotent Stem Cell Neurons

Cited by 39 publications

References 34 publications

Common developmental genome deprogramming in schizophrenia — Role of Integrative Nuclear FGFR1 Signaling (INFS)

Common developmental genome deprogramming in schizophrenia — Role of Integrative Nuclear FGFR1 Signaling (INFS)

Tracing Early Neurodevelopment in Schizophrenia with Induced Pluripotent Stem Cells

Prefrontal co-expression of schizophrenia risk genes is associated with treatment response in patients

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