Abstract

The adverse effects of prenatal alcohol on the developing central nervous system (CNS) have been well documented and may be permanent in nature, resulting in limited mental capabilities and abnormal behavior. The substrates for these abnormalities are unknown, although cell loss and alterations in neuronal structure have been implicated in studies with animal models. The physiological consequences of these alterations are unknown. In the present proposal a continuation proposal, a culture model system, electrophysiological techniques and a chronic exposure paradigm will be used to identify alcohol induced alterations in the functional properties of CNS neurons that may be the basis for the neurotoxic effects of alcohol in the developing CNS. An identified CNS neuronal type, the cerebellar Purkinje neuron, which is a sensitive and favorable model for alcohol studies in adult animals is the experimental model. the properties to be examined include the postsynaptic mechanisms mediating sensitivity to chemical transmitters and the ionic conductances mediating electrical excitability. Studies completed during the first funding period implicated these mechanisms as target sites of chronic alcohol action in developing Purkinje neurons. Alterations in these properties will be assessed with extracellular and intracellular recording techniques. The site and mechanisms of alcohol action will be determined with voltage-clamp and single channel recording techniques. This approach will provide information at the cellular, membrane and molecular levels and is required to unequivocally identify the sites and mechanisms of alcohol action. Because of the large somatic and dendritic structure of the Purkinje neuron, it will be possible to carry out these studies in both cellular regions. The use of a culture system offers considerable technical advantage and makes it possible to expose the developing neurons to known and stable concentrations of alcohol. This approach minimizes interpretiative problems related to questions of alcohol distribution, actions of metabolic products, nutritional deficits and indirect effects via other sensitive brain regions. The proposed experiments represent a novel and state of the art approach to the study of chronic alcohol actions on CNS neuronal physiology and development. The resulting data should contribute significantly to our understanding of the neurotoxic actions of chronic alcohol on neuronal development and function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA006665-06
Application #
3109947
Study Section
Biochemistry, Physiology and Medicine Subcommittee (ALCB)
Project Start
1985-06-01
Project End
1993-11-30
Budget Start
1990-12-01
Budget End
1991-11-30
Support Year
6
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Netzeband, Jeffrey G; Schneeloch, Jaimes R; Trotter, Carol et al. (2002) Chronic ethanol treatment and withdrawal alter ACPD-evoked calcium signals in developing Purkinje neurons. Alcohol Clin Exp Res 26:386-93
Liljelund, P; Netzeband, J G; Gruol, D L (2000) L-Type calcium channels mediate calcium oscillations in early postnatal Purkinje neurons. J Neurosci 20:7394-403
Netzeband, J G; Trotter, C; Parsons, K L et al. (1999) Chronic ethanol treatment alters AMPA-induced calcium signals in developing Purkinje neurons. Brain Res 826:270-80
Netzeband, J G; Trotter, C; Caguioa, J N et al. (1999) Chronic ethanol exposure enhances AMPA-elicited Ca2+ signals in the somatic and dendritic regions of cerebellar Purkinje neurons. Neurochem Int 35:163-74
Gruol, D L; Ryabinin, A E; Parsons, K L et al. (1998) Neonatal alcohol exposure reduces NMDA induced Ca2+ signaling in developing cerebellar granule neurons. Brain Res 793:12-20
Gruol, D L; Netzeband, J G; Parsons, K L (1996) Ca2+ signaling pathways linked to glutamate receptor activation in the somatic and dendritic regions of cultured cerebellar purkinje neurons. J Neurophysiol 76:3325-40
Gruol, D L; Parsons, K L (1996) Chronic alcohol reduces calcium signaling elicited by glutamate receptor stimulation in developing cerebellar neurons. Brain Res 728:166-74
Gruol, D L; Curry, J G (1995) Calcium signals elicited by quisqualate in cultured Purkinje neurons show developmental changes in sensitivity to acute alcohol. Brain Res 673:1-12
Gruol, D L; Parsons, K L (1994) Chronic exposure to alcohol during development alters the calcium currents of cultured cerebellar Purkinje neurons. Brain Res 634:283-90
Gruol, D L (1992) Chronic exposure to alcohol during development alters the responses to excitatory amino acids in cultured Purkinje neurons. Brain Res 574:271-9

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