Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia

Brennand, Kristen J.; Savas, Jeffrey N.; Kim, Yoonsoo; Tran, N.; Simone, Anthony; Hashimoto-Torii, Kazue; Beaumont, Kristin G.; Kim, H. J.; Topol, Aaron; Ladran, Ian; Abdelrahim, Mohammed; Matikainen‐Ankney, Bridget A.; Chao, Shih-Hui; Mrksich, Milan; Rakić, Paško; Fang, Gang; Zhang, Bin; Yates, John R.; Gage, Fred H.

doi:10.1038/mp.2014.22

Cited by 365 publications

(411 citation statements)

References 32 publications

Supporting

Mentioning

380

Contrasting

Order By: Relevance

“…Though NPCs appear to be morphologically similar by eye, they are a heterogeneous population comprised of cells capable of generating both glutamatergic and GABAergic neurons. While we observe remarkably consistent forebrain patterning of NPC lines between individuals using this method 1 , this is only when comparing fully validated high quality NPC lines -there are substantial differences between good and poor quality NPC lines. Additionally, viral transduction yields genetically heterogeneous cells, each with an integration of the viral vector at a unique genomic location; therefore, individual cells will vary both in the location and number of genomic integration sites.…”

Section: Discussionmentioning

confidence: 92%

“…Furthermore, because one can rapidly generate large numbers of cells and need not wait weeks or months for neuronal maturation, NPC-based assays are suitable for the study of larger patient cohorts and are more amenable to high throughput screening. We believe that hiPSC NPCs can serve as a proxy for the developmental pathways potentially contributing to disease pathogenesis, as has already been demonstrated in disorders as diverse as schizophrenia 1 and Huntington's disease 11 .…”

Section: Introductionmentioning

confidence: 99%

“…Gene expression studies of neurons differentiated in vitro from human induced pluripotent stem cells (hiPSCs) by us 1 and others 2,3 indicate that hiPSC neurons resemble fetal rather than adult brain tissue. At present, hiPSC-based models may be more appropriate for the study of predisposition to, rather than late features of, neurological disease.…”

Section: Introductionmentioning

confidence: 99%

“…We have previously reported that a significant fraction of the gene signature of schizophrenia hiPSC-derived neurons is conserved in schizophrenia hiPSC-derived neural progenitor cells (NPCs), indicating that NPCs may be a useful cell type for studying the molecular pathways contributing to schizophrenia 1 . We and others have reported aberrant migration, increased oxidative stress and reactive oxygen species, sensitivity to sub-threshold environmental stresses and impaired mitochondrial function in schizophrenia hiPSC NPCs 1,[4][5][6] , as well as decreased neuronal connectivity and synaptic function in schizophrenia hiPSC neurons 5,[7][8][9][10] . If the molecular factors contributing to aberrant migration and/or oxidative stress in schizophrenia hiPSC NPCs also underlie the reduced neuronal connectivity in schizophrenia hiPSC-derived neurons, NPCs could be a robust and highly replicative neural population with which to study the mechanisms responsible for disease.…”

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

A Guide to Generating and Using hiPSC Derived NPCs for the Study of Neurological Diseases

Topol

Tran

Brennand

2015

JoVE

View full text Add to dashboard Cite

Post-mortem studies of neurological diseases are not ideal for identifying the underlying causes of disease initiation, as many diseases include a long period of disease progression prior to the onset of symptoms. Because fibroblasts from patients and healthy controls can be efficiently reprogrammed into human induced pluripotent stem cells (hiPSCs), and subsequently differentiated into neural progenitor cells (NPCs) and neurons for the study of these diseases, it is now possible to recapitulate the developmental events that occurred prior to symptom onset in patients. We present a method by which to efficiently differentiate hiPSCs into NPCs, which in addition to being capable of further differentiation into functional neurons, can also be robustly passaged, freeze-thawed or transitioned to grow as neurospheres, enabling rapid genetic screening to identify the molecular factors that impact cellular phenotypes including replication, migration, oxidative stress and/or apoptosis. Patient derived hiPSC NPCs are a unique platform, ideally suited for the empirical testing of the cellular or molecular consequences of manipulating gene expression. Video LinkThe video component of this article can be found at

show abstract

Section: Discussionmentioning

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

A Guide to Generating and Using hiPSC Derived NPCs for the Study of Neurological Diseases

Topol

Tran

Brennand

2015

JoVE

View full text Add to dashboard Cite

show abstract

“…Direct reprogramming of somatic cells into a target cell type by forced expression of reprogramming factors without going through an intermediate iPS cell state is a very powerful tool for disease modelling because of the ability to generate specific mature human somatic cells within a short period of time. Our laboratory has demonstrated that fibroblasts could be directly converted into functional mature neuronal cells within two weeks, whereas conventional differentiation of pluripotent cells into somatic lineages (such as neural, hematopoietic, cardiac and hepatic) through exposure to morphogens and small molecules produces cells that are typically immature, resembling fetal stages [72]. Even maturation times of several months are often insufficient to generate mature, adult-like cell types from pluripotent stem cells.…”

Section: Direct Conversion Of Somatic Cells Versus Induction Of Plurimentioning

confidence: 99%

Direct somatic lineage conversion

Tanabe¹,

Haag²,

Wernig³

2015

Phil. Trans. R. Soc. B

View full text Add to dashboard Cite

The predominant view of embryonic development and cell differentiation has been that rigid and even irreversible epigenetic marks are laid down along the path of cell specialization ensuring the proper silencing of unrelated lineage programmes. This model made the prediction that specialized cell types are stable and cannot be redirected into other lineages. Accordingly, early attempts to change the identity of somatic cells had little success and was limited to conversions between closely related cell types. Nuclear transplantation experiments demonstrated, however, that specialized cells even from adult mammals can be reprogrammed into a totipotent state. The discovery that a small combination of transcription factors can reprogramme cells to pluripotency without the need of oocytes further supported the view that these epigenetic barriers can be overcome much easier than assumed, but the extent of this flexibility was still unclear. When we showed that a differentiated mesodermal cell can be directly converted to a differentiated ectodermal cell without a pluripotent intermediate, it was suggested that in principle any cell type could be converted into any other cell type. Indeed, the work of several groups in recent years has provided many more examples of direct somatic lineage conversions. Today, the question is not anymore whether a specific cell type can be generated by direct reprogramming but how it can be induced.

show abstract

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

et al. 2016

View full text Add to dashboard Cite

IMPORTANCE Schizophrenia candidate genes participate in common molecular pathways that are regulated by activity-dependent changes in neurons. One important next step is to further our understanding on the role of activity-dependent changes of genes expression in the etiopathogenesis of schizophrenia. OBJECTIVE To examine whether neuronal activity-dependent changes of gene expression is dysregulated in schizophrenia. DESIGN, SETTING, AND PARTICIPANTS Neurons differentiated from human induced pluripotent stem cells (hiPSCs) derived from 4 cases with schizophrenia and 4 unaffected controls were depolarized using potassium chloride. RNA was extracted followed by genome-wide profiling of the transcriptome. MAIN OUTCOMES AND MEASURES We performed differential expression analysis and gene co-expression analysis to identify activity-dependent or disease-specific changes of the transcriptome. Gene expression differences were assessed with linear models. Further, we used gene set analyses to identify co-expressed modules that are enriched for schizophrenia risk genes. RESULTS We identified 1,669 genes that are significantly different in schizophrenia-associated vs. control hiPSC-derived neurons and 1,199 genes that are altered in these cells in response to depolarization (linear models at false discovery rate ≤ 0.05). We show that the effect of activity-dependent changes of gene expression in schizophrenia-associated neurons (59 significant genes at false discovery rate ≤ 0.05) is attenuated compared to controls (594 significant genes at false discovery rate ≤ 0.05). Using gene co-expression analysis, we identified 2 modules (turquoise and brown) that are associated with diagnosis status and 2 modules (yellow and green) that are associated with depolarization at false discovery rate ≤ 0.05. For 3 out of the 4 modules we found enrichment with schizophrenia-associated variants: brown (Fisher’s P = 0.002), turquoise (Fisher’s P = 0.044) and yellow (Fisher’s P = 0.018). CONCLUSIONS AND RELEVANCE Our results show that schizophrenia candidate genes cluster within gene networks that are associated with a blunted effect of activity-dependent changes of gene expression in schizophrenia-associated neurons. Overall, these findings link schizophrenia candidate genes with specific molecular functions in neurons, which could be utilized to examine underlying mechanisms and therapeutic interventions related to schizophrenia.

show abstract

Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia

Cited by 365 publications

References 32 publications

A Guide to Generating and Using hiPSC Derived NPCs for the Study of Neurological Diseases

A Guide to Generating and Using hiPSC Derived NPCs for the Study of Neurological Diseases

Direct somatic lineage conversion

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

Contact Info

Product

Resources

About