Abstract

Multiple lines of evidence implicate dysfunction of cerebral cortical inhibitory interneurons in the symptomatology of major neuropsychiatric illnesses, including schizophrenia, autism, Tourette disorder, bipolar disorder, and epilepsy. This dysfunction involves subtypes of interneurons that differ in their neurochemistry, connectivity, and physiological characteristics. Recent advances in the derivation of interneurons from human pluripotent stem cells (PSCs) demonstrate their utility in studies of neuronal developmental genetics, function, and disease. Unfortunately, there has been limited success at generating the parvalbumin-expressing, fast- spiking (PV-FS) subgroup, even though this is the most plentiful subgroup of cortical interneuron and their dysfunction is strongly implicated neuropsychiatric disease. Despite tremendous progress in enriching for mouse embryonic stem cell (mESC)-derived PV-FS interneurons, no approach for enriching for their human counterparts is available. This shortfall may be secondary to the length and complexity of human forebrain neural subtype-specific directed differentiation protocols, but also to the protracted maturation of PV-FS cells that normally require strong excitatory inputs to mature. The goal of this highly focused, 3-year, modular budget, renewal application is to build directly upon our substantial progress in deriving PV-FS from mESCs the previous grant cycle, together with our progress at accelerating the maturation of human stem cell derived interneuron-like cells by conditional activation of mTOR signaling, to enrich for the derivation of PV-FS interneurons from human PSCs. Through this scalable process we will also establish experimental systems, including co-culture with prenatal rat cortical neurons and astrocytes, transplantation into neonatal mouse neocortex, and engraftment into human forebrain organoids, that will enable complimentary scientific questions to be addressed. Success in this endeavor will make possible a host of future studies on the etiology, prevention, and treatment of interneuron-related neuropsychiatric disease.

Public Health Relevance

Multiple lines of evidence implicate dysfunction of cerebral cortical inhibitory interneurons in the symptomatology of major neuropsychiatric illnesses. Human stem cell derived neurons have become an invaluable resource for the study and treatment of brain disease, but thus far it has not been possible to enrich for the generation of the most frequently disease associated subclass of cortical interneuron, the parvalbumin expressing fast-spiking cell. This renewal application builds on our recent progress, both in the generation of parvalbumin-expressing fast-spiking interneurons from mouse stem cells, and in the acceleration of human stem cell derived interneuron maturation, to create scalable approaches for the generation of this critical neuronal subclass from human stem cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH066912-16
Application #
9720929
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Panchision, David M
Project Start
2003-01-01
Project End
2021-03-31
Budget Start
2019-04-01
Budget End
2020-03-31
Support Year
16
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Children's Hospital of Philadelphia
Department
Type
DUNS #
073757627
City
Philadelphia
State
PA
Country
United States
Zip Code
19146

  Publications

Tischfield, David J; Anderson, Stewart A (2017) Differentiation of Mouse Embryonic Stem Cells into Cortical Interneuron Precursors. J Vis Exp :
Donegan, J J; Tyson, J A; Branch, S Y et al. (2017) Stem cell-derived interneuron transplants as a treatment for schizophrenia: preclinical validation in a rodent model. Mol Psychiatry 22:1492-1501
Tischfield, David J; Saraswat, Dave K; Furash, Andrew et al. (2017) Loss of the neurodevelopmental gene Zswim6 alters striatal morphology and motor regulation. Neurobiol Dis 103:174-183
Tischfield, David J; Kim, Junho; Anderson, Stewart A (2017) Atypical PKC and Notch Inhibition Differentially Modulate Cortical Interneuron Subclass Fate from Embryonic Stem Cells. Stem Cell Reports 8:1135-1143
Dimidschstein, Jordane; Chen, Qian; Tremblay, Robin et al. (2016) A viral strategy for targeting and manipulating interneurons across vertebrate species. Nat Neurosci 19:1743-1749
Jaiswal, Manoj K; Keros, Sotirios; Zhao, Mingrui et al. (2015) Reduction in focal ictal activity following transplantation of MGE interneurons requires expression of the GABAA receptor ?4 subunit. Front Cell Neurosci 9:127
Tyson, Jennifer A; Goldberg, Ethan M; Maroof, Asif M et al. (2015) Duration of culture and sonic hedgehog signaling differentially specify PV versus SST cortical interneuron fates from embryonic stem cells. Development 142:1267-78
Blazquez-Llorca, Lidia; Woodruff, Alan; Inan, Melis et al. (2015) Spatial distribution of neurons innervated by chandelier cells. Brain Struct Funct 220:2817-34
Li, Deqiang; Takeda, Norifumi; Jain, Rajan et al. (2015) Hopx distinguishes hippocampal from lateral ventricle neural stem cells. Stem Cell Res 15:522-529
Petros, Timothy J; Bultje, Ronald S; Ross, M Elizabeth et al. (2015) Apical versus Basal Neurogenesis Directs Cortical Interneuron Subclass Fate. Cell Rep 13:1090-1095

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