Identification and characterization of neuronal precursors and their progeny from human fetal tissue.
Study Design
- Studientyp
- In Vitro
- Population
- Human fetal brain tissue (18-22 weeks)
- Intervention
- Identification and characterization of neuronal precursors and their progeny from human fetal tissue. None
- Vergleichsgruppe
- None
- Primärer Endpunkt
- Neuronal precursor identification in human fetal brain
- Wirkungsrichtung
- Mixed
- Verzerrungsrisiko
- Unclear
Abstract
We have examined primary human neuronal precursors (HNPs) from 18-22-week-old fetuses. We showed that E-NCAM/MAP2/beta-III tubulin-immunoreactive neuronal precursors divide in vitro and could be induced to differentiate into mature neurons in 2 weeks. HNPs did not express nestin and differentiated slowly compared to rodent neuronal restricted precursors (NRPs, 5 days). Immunocytochemical and physiological analyses showed that HNPs could generate a heterogeneous population of neurons that expressed neurofilament-associated protein and various neurotransmitters, neurotransmitter synthesizing enzymes, voltage-gated ion channels, and ligand-gated neurotransmitter receptors and could fire action potentials. Undifferentiated and differentiated HNPs did not coexpress glial markers. Only a subset of cells that expressed GFP under the control of the Talpha1 tubulin promoter was E-NCAM/beta-III tubulin-immunoreactive, indicating nonexclusive overlap between these two HNP cell populations. Overall, HNPs resemble NRPs isolated from rodent tissue and appear to be a neuronal precursor population.
Zusammenfassung
Overall, HNPs resemble NRPs isolated from rodent tissue and appear to be a neuronal precursor population.
Used In Evidence Reviews
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