Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia

K. Brennand; J. N. Savas; Y. Kim; N. Tran; A. Simone; K. Hashimoto-Torii; K. G. Beaumont; H. J. Kim; A. Topol; I. Ladran; M. Abdelrahim; B. Matikainen-Ankney; S. H. Chao; M. Mrksich; P. Rakic; G. Fang; B. Zhang; J. R. Yates; F. H. Gage

doi:10.1038/mp.2014.22

Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia

K. Brennand^*, J. N. Savas, Y. Kim, N. Tran, A. Simone, K. Hashimoto-Torii, K. G. Beaumont, H. J. Kim, A. Topol, I. Ladran, M. Abdelrahim, B. Matikainen-Ankney, S. H. Chao, M. Mrksich, P. Rakic, G. Fang, B. Zhang, J. R. Yates, F. H. Gage

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

287 Scopus citations

Abstract

Consistent with recent reports indicating that neurons differentiated in vitro from human-induced pluripotent stem cells (hiPSCs) are immature relative to those in the human brain, gene expression comparisons of our hiPSC-derived neurons to the Allen BrainSpan Atlas indicate that they most resemble fetal brain tissue. This finding suggests that, rather than modeling the late features of schizophrenia (SZ), hiPSC-based models may be better suited for the study of disease predisposition. We now report that a significant fraction of the gene signature of SZ hiPSC-derived neurons is conserved in SZ hiPSC neural progenitor cells (NPCs). We used two independent discovery-based approaches - microarray gene expression and stable isotope labeling by amino acids in cell culture (SILAC) quantitative proteomic mass spectrometry analyses - to identify cellular phenotypes in SZ hiPSC NPCs from four SZ patients. From our findings that SZ hiPSC NPCs show abnormal gene expression and protein levels related to cytoskeletal remodeling and oxidative stress, we predicted, and subsequently observed, aberrant migration and increased oxidative stress in SZ hiPSC NPCs. These reproducible NPC phenotypes were identified through scalable assays that can be applied to expanded cohorts of SZ patients, making them a potentially valuable tool with which to study the developmental mechanisms contributing to SZ.

Original language	English (US)
Pages (from-to)	361-368
Number of pages	8
Journal	Molecular Psychiatry
Volume	20
Issue number	3
DOIs	https://doi.org/10.1038/mp.2014.22
State	Published - Mar 12 2015

ASJC Scopus subject areas

Psychiatry and Mental health
Cellular and Molecular Neuroscience
Molecular Biology

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10.1038/mp.2014.22

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Brennand, K., Savas, J. N., Kim, Y., Tran, N., Simone, A., Hashimoto-Torii, K., Beaumont, K. G., Kim, H. J., Topol, A., Ladran, I., Abdelrahim, M., Matikainen-Ankney, B., Chao, S. H., Mrksich, M., Rakic, P., Fang, G., Zhang, B., Yates, J. R., & Gage, F. H. (2015). Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia. Molecular Psychiatry, 20(3), 361-368. https://doi.org/10.1038/mp.2014.22

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title = "Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia",

abstract = "Consistent with recent reports indicating that neurons differentiated in vitro from human-induced pluripotent stem cells (hiPSCs) are immature relative to those in the human brain, gene expression comparisons of our hiPSC-derived neurons to the Allen BrainSpan Atlas indicate that they most resemble fetal brain tissue. This finding suggests that, rather than modeling the late features of schizophrenia (SZ), hiPSC-based models may be better suited for the study of disease predisposition. We now report that a significant fraction of the gene signature of SZ hiPSC-derived neurons is conserved in SZ hiPSC neural progenitor cells (NPCs). We used two independent discovery-based approaches - microarray gene expression and stable isotope labeling by amino acids in cell culture (SILAC) quantitative proteomic mass spectrometry analyses - to identify cellular phenotypes in SZ hiPSC NPCs from four SZ patients. From our findings that SZ hiPSC NPCs show abnormal gene expression and protein levels related to cytoskeletal remodeling and oxidative stress, we predicted, and subsequently observed, aberrant migration and increased oxidative stress in SZ hiPSC NPCs. These reproducible NPC phenotypes were identified through scalable assays that can be applied to expanded cohorts of SZ patients, making them a potentially valuable tool with which to study the developmental mechanisms contributing to SZ.",

author = "K. Brennand and Savas, {J. N.} and Y. Kim and N. Tran and A. Simone and K. Hashimoto-Torii and Beaumont, {K. G.} and Kim, {H. J.} and A. Topol and I. Ladran and M. Abdelrahim and B. Matikainen-Ankney and Chao, {S. H.} and M. Mrksich and P. Rakic and G. Fang and B. Zhang and Yates, {J. R.} and Gage, {F. H.}",

note = "Funding Information: L Moore, B Miller, K Stecker, A Patruno, J Rose, E Xia and S Larkin provided technical assistance. The Salk Stem Cell facility, the Salk Viral Vector Core and the Icahn School of Medicine Stem Cell Core all provided support. J Nguyen and L Ouyang provided gene expression support. D Chambers provided FACS support, ML Gage provided editorial comments. We thank M McConnell, C Marchetto and L Boyer for their advice and conversation. The Gage Laboratory is partially funded by California Institute of Regenerative Medicine (CIRM) grant RL1-00649-1, the G Harold & Leila Y Mathers Foundation, the JPB Foundation, the Leona M and Harry B Helmsley Charitable Trust, Annette Merle-Smith, and Robert and Mary Jane Engman. Kristen Brennand is a New York Stem Cell Foundation—Robertson Investigator. The Brennand Laboratory is supported by a Brain and Behavior Young Investigator Grant, National Institute of Health (NIH) grant R01 MH101454 and the New York Stem Cell Foundation. The Yates laboratory is supported by NIH grants R01 MH068770, P41 GM103533 and R01MH100175, while JNS is supported by National Research Service Award (NRSA) fellowship F32 AG039127 and F Hoffman-La Roche Postdoctoral Fellowship Award SFP2063. The Rakic laboratory is supported by NIH grants R01 DA023999 and R01 NS014841, and the Kavli Institute for Neuroscience at Yale. The Hashimoto-Torii laboratory is funded by NARSAD, CTSI-CN and R00 AA018387. The Zhang laboratory is supported by R01 AG046170, R21 MH097156-01A1, R01 CA163772 and U01AI111598-01. The Mrksich laboratory is funded by the Chicago Biomedical Consortium with support from the Searle Funds at The Chicago Community Trust. Publisher Copyright: {\textcopyright} 2015 Macmillan Publishers Limited.",

year = "2015",

month = mar,

day = "12",

doi = "10.1038/mp.2014.22",

language = "English (US)",

volume = "20",

pages = "361--368",

journal = "Molecular Psychiatry",

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Brennand, K, Savas, JN, Kim, Y, Tran, N, Simone, A, Hashimoto-Torii, K, Beaumont, KG, Kim, HJ, Topol, A, Ladran, I, Abdelrahim, M, Matikainen-Ankney, B, Chao, SH, Mrksich, M, Rakic, P, Fang, G, Zhang, B, Yates, JR & Gage, FH 2015, 'Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia', Molecular Psychiatry, vol. 20, no. 3, pp. 361-368. https://doi.org/10.1038/mp.2014.22

TY - JOUR

T1 - Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia

AU - Brennand, K.

AU - Savas, J. N.

AU - Kim, Y.

AU - Tran, N.

AU - Simone, A.

AU - Hashimoto-Torii, K.

AU - Beaumont, K. G.

AU - Kim, H. J.

AU - Topol, A.

AU - Ladran, I.

AU - Abdelrahim, M.

AU - Matikainen-Ankney, B.

AU - Chao, S. H.

AU - Mrksich, M.

AU - Rakic, P.

AU - Fang, G.

AU - Zhang, B.

AU - Yates, J. R.

AU - Gage, F. H.

N1 - Funding Information: L Moore, B Miller, K Stecker, A Patruno, J Rose, E Xia and S Larkin provided technical assistance. The Salk Stem Cell facility, the Salk Viral Vector Core and the Icahn School of Medicine Stem Cell Core all provided support. J Nguyen and L Ouyang provided gene expression support. D Chambers provided FACS support, ML Gage provided editorial comments. We thank M McConnell, C Marchetto and L Boyer for their advice and conversation. The Gage Laboratory is partially funded by California Institute of Regenerative Medicine (CIRM) grant RL1-00649-1, the G Harold & Leila Y Mathers Foundation, the JPB Foundation, the Leona M and Harry B Helmsley Charitable Trust, Annette Merle-Smith, and Robert and Mary Jane Engman. Kristen Brennand is a New York Stem Cell Foundation—Robertson Investigator. The Brennand Laboratory is supported by a Brain and Behavior Young Investigator Grant, National Institute of Health (NIH) grant R01 MH101454 and the New York Stem Cell Foundation. The Yates laboratory is supported by NIH grants R01 MH068770, P41 GM103533 and R01MH100175, while JNS is supported by National Research Service Award (NRSA) fellowship F32 AG039127 and F Hoffman-La Roche Postdoctoral Fellowship Award SFP2063. The Rakic laboratory is supported by NIH grants R01 DA023999 and R01 NS014841, and the Kavli Institute for Neuroscience at Yale. The Hashimoto-Torii laboratory is funded by NARSAD, CTSI-CN and R00 AA018387. The Zhang laboratory is supported by R01 AG046170, R21 MH097156-01A1, R01 CA163772 and U01AI111598-01. The Mrksich laboratory is funded by the Chicago Biomedical Consortium with support from the Searle Funds at The Chicago Community Trust. Publisher Copyright: © 2015 Macmillan Publishers Limited.

PY - 2015/3/12

Y1 - 2015/3/12

N2 - Consistent with recent reports indicating that neurons differentiated in vitro from human-induced pluripotent stem cells (hiPSCs) are immature relative to those in the human brain, gene expression comparisons of our hiPSC-derived neurons to the Allen BrainSpan Atlas indicate that they most resemble fetal brain tissue. This finding suggests that, rather than modeling the late features of schizophrenia (SZ), hiPSC-based models may be better suited for the study of disease predisposition. We now report that a significant fraction of the gene signature of SZ hiPSC-derived neurons is conserved in SZ hiPSC neural progenitor cells (NPCs). We used two independent discovery-based approaches - microarray gene expression and stable isotope labeling by amino acids in cell culture (SILAC) quantitative proteomic mass spectrometry analyses - to identify cellular phenotypes in SZ hiPSC NPCs from four SZ patients. From our findings that SZ hiPSC NPCs show abnormal gene expression and protein levels related to cytoskeletal remodeling and oxidative stress, we predicted, and subsequently observed, aberrant migration and increased oxidative stress in SZ hiPSC NPCs. These reproducible NPC phenotypes were identified through scalable assays that can be applied to expanded cohorts of SZ patients, making them a potentially valuable tool with which to study the developmental mechanisms contributing to SZ.

AB - Consistent with recent reports indicating that neurons differentiated in vitro from human-induced pluripotent stem cells (hiPSCs) are immature relative to those in the human brain, gene expression comparisons of our hiPSC-derived neurons to the Allen BrainSpan Atlas indicate that they most resemble fetal brain tissue. This finding suggests that, rather than modeling the late features of schizophrenia (SZ), hiPSC-based models may be better suited for the study of disease predisposition. We now report that a significant fraction of the gene signature of SZ hiPSC-derived neurons is conserved in SZ hiPSC neural progenitor cells (NPCs). We used two independent discovery-based approaches - microarray gene expression and stable isotope labeling by amino acids in cell culture (SILAC) quantitative proteomic mass spectrometry analyses - to identify cellular phenotypes in SZ hiPSC NPCs from four SZ patients. From our findings that SZ hiPSC NPCs show abnormal gene expression and protein levels related to cytoskeletal remodeling and oxidative stress, we predicted, and subsequently observed, aberrant migration and increased oxidative stress in SZ hiPSC NPCs. These reproducible NPC phenotypes were identified through scalable assays that can be applied to expanded cohorts of SZ patients, making them a potentially valuable tool with which to study the developmental mechanisms contributing to SZ.

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Phenotypic differences in hiPSC NPCs derived from patients with schizophrenia

Abstract

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