Abstract

The research outlined in this portion of the program project is designed to define the putative excitatory amino acid transmitters and receptors associated with cerebellar afferent systems in normal rats. Although neurotransmitters in the majority of cerebellar cortical neurons have been identified, information on the transmitters of cerebellar climbing fibers remains controversial and the major transmitters of the mossy fibers have yet to be defined. The experiments proposed will examine several acidic amino acid compounds, nitric oxide and polyamines as possible transmitter candidates for the olivocerebellar pathway and selected mossy fiber pathways. This research will provide basic information relevant to our understanding of the biochemical and pharmacological characteristics of cerebellar afferent systems. Our proposed investigation is described by the following three specific aims: 1. To determine whether glutamate, aspartate, NAAG, nitric oxide synthase or spermidine and putresine immunoreactivity is associated with identified climbing fiber or mossy fiber terminals by employing anterograde tracing with PHA-L and biotinylated dextran amine (BDA) in combination with immunocytochemistry at both light and electron microscopic levels. 2. Based on the results of 1, we will ascertain whether aspartate, glutamate, NAAG, citrulline, spermine or putresine are released in the cerebellar cortex following olivary, vestibular, LRN or middle cerebellar peduncle stimulation by combining electrical or chemical stimulation with in vivo microdialysis and electrophysiological recording or C-fos immunostaining. 3. The types of excitatory amino acid receptors associated with cerebellar afferents will be defined using: A) direct ultrastructural examination of PHA-L or BDA labeled terminals in combination with immunocytochemical localization of glutamate receptor subtypes and B) lesions of selected afferent pathways will be employed in combination with immunoprecipitation techniques and in situ hybridization.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
5P01NS031318-04
Application #
5215418
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
4
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Kuceyeski, Amy; Navi, Babak B; Kamel, Hooman et al. (2016) Structural connectome disruption at baseline predicts 6-months post-stroke outcome. Hum Brain Mapp 37:2587-601
Chen, Gang; Gao, Wangcai; Reinert, Kenneth C et al. (2005) Involvement of kv1 potassium channels in spreading acidification and depression in the cerebellar cortex. J Neurophysiol 94:1287-98
Goswami, Jaideep; Martin, Loren A; Goldowitz, Daniel et al. (2005) Enhanced Purkinje cell survival but compromised cerebellar function in targeted anti-apoptotic protein transgenic mice. Mol Cell Neurosci 29:202-21
Brodie, Christopher R; Khaliq, Mahmooda; Yin, Jerry C P et al. (2004) Overexpression of CREB reduces CRE-mediated transcription: behavioral and cellular analyses in transgenic mice. Mol Cell Neurosci 25:602-11
Reinert, Kenneth C; Dunbar, Robert L; Gao, Wangcai et al. (2004) Flavoprotein autofluorescence imaging of neuronal activation in the cerebellar cortex in vivo. J Neurophysiol 92:199-211
Dunbar, R L; Chen, G; Gao, W et al. (2004) Imaging parallel fiber and climbing fiber responses and their short-term interactions in the mouse cerebellar cortex in vivo. Neuroscience 126:213-27
Beitz, Alvin J; Saxon, Dale (2004) Harmaline-induced climbing fiber activation causes amino acid and peptide release in the rodent cerebellar cortex and a unique temporal pattern of Fos expression in the olivo-cerebellar pathway. J Neurocytol 33:49-74
Zhang, Yi; Forster, Colleen; Milner, Teresa A et al. (2003) Attenuation of activity-induced increases in cerebellar blood flow by lesion of the inferior olive. Am J Physiol Heart Circ Physiol 285:H1177-82
Yang, Guang; Zhang, Yi; Ross, M Elizabeth et al. (2003) Attenuation of activity-induced increases in cerebellar blood flow in mice lacking neuronal nitric oxide synthase. Am J Physiol Heart Circ Physiol 285:H298-304
Gao, Wangcai; Dunbar, Robert L; Chen, Gang et al. (2003) Optical imaging of long-term depression in the mouse cerebellar cortex in vivo. J Neurosci 23:1859-66

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