Abstract

Visual experience modulates the development circuits in the brain that process visual information. One way that such neuronal activity can modify neuronal development is by changing the structure of the component parts, the individual neurons themselves. Considerable evidence supports the hypothesis that neuronal growth can be increased or decreased by changes in the pattern of electrical activity experienced by the neuron. The biochemical mechanisms by which such changes in neuronal growth occur are likely to be mediated through enzymes which themselves are controlled by neuronal activity. One such class of enzymes is the calcium-sensitive protein kinases, including. This protein kinase has been implicated in neuronal development, synapse formation and synaptic plasticity in the visual system. Unfortunately the pharmacological agents used in earlier studies could not clearly distinguish CaMKII and another calcium-sensitive protein kinase, protein kinases C. To address the problem of poor specificity of pharmacological agents, we now propose to use Vaccinia virus to introduce into neurons of the frog visual system a gene for a form of CaMKII that is no longer regulated by calcium and calmodulin. With this method, we can obtain expression of the constitutively active kinase only in the postsynaptic neurons, but not in the presynaptic retinal cells. Using confocal microscopy, we will then take time-lapse images of dye-labeled retinal axons or optic tectal neurons to observe their pattern of growth over a period of up to 4 days This latter method offers the unique opportunity to observe neurons grow in their normal complex environment. Previous experiments in fixed tissue have provided static images of neuronal development, from which active processes were inferred. Thus far, our observations of neuronal growth in situ have shown that in fact neuronal structure is much more dynamic than previously recognized and that retinal axonal structure can be modified by activity at earlier developmental stages than previously thought. By combining these 2 techniques, viral transfection of neurons in the optic tectum and confocal imaging of developing neurons in situ we will be able to test the hypothesis that postsynaptic CaMKII activity can modify the development of neuronal structure and synaptic circuits in the visual system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY011261-06
Application #
6329551
Study Section
Special Emphasis Panel (ZRG1-VISA (02))
Program Officer
Oberdorfer, Michael
Project Start
1995-12-06
Project End
2004-11-30
Budget Start
2000-12-01
Budget End
2001-11-30
Support Year
6
Fiscal Year
2001
Total Cost
$438,640
Indirect Cost

  Institution

Name
Cold Spring Harbor Laboratory
Department
Type
DUNS #
065968786
City
Cold Spring Harbor
State
NY
Country
United States
Zip Code
11724

  Publications

Liu, Han-Hsuan; McClatchy, Daniel B; Schiapparelli, Lucio et al. (2018) Role of the visual experience-dependent nascent proteome in neuronal plasticity. Elife 7:
Gambrill, Abigail C; Faulkner, Regina L; McKeown, Caroline R et al. (2018) Enhanced visual experience rehabilitates the injured brain in Xenopus tadpoles in an NMDAR-dependent manner. J Neurophysiol :
Gambrill, Abigail C; Faulkner, Regina L; Cline, Hollis T (2018) Direct intertectal inputs are an integral component of the bilateral sensorimotor circuit for behavior in Xenopus tadpoles. J Neurophysiol 119:1947-1961
He, Hai-Yan; Shen, Wanhua; Zheng, Lijun et al. (2018) Excitatory synaptic dysfunction cell-autonomously decreases inhibitory inputs and disrupts structural and functional plasticity. Nat Commun 9:2893
McKeown, C R; Thompson, C K; Cline, H T (2017) Reversible developmental stasis in response to nutrient availability in the Xenopus laevis central nervous system. J Exp Biol 220:358-368
Lau, Melissa; Li, Jianli; Cline, Hollis T (2017) In Vivo Analysis of the Neurovascular Niche in the Developing Xenopus Brain. eNeuro 4:
Pratt, Kara G; Hiramoto, Masaki; Cline, Hollis T (2016) An Evolutionarily Conserved Mechanism for Activity-Dependent Visual Circuit Development. Front Neural Circuits 10:79
He, Hai-Yan; Shen, Wanhua; Hiramoto, Masaki et al. (2016) Experience-Dependent Bimodal Plasticity of Inhibitory Neurons in Early Development. Neuron 90:1203-1214
Thompson, Christopher K; Cline, Hollis T (2016) Thyroid Hormone Acts Locally to Increase Neurogenesis, Neuronal Differentiation, and Dendritic Arbor Elaboration in the Tadpole Visual System. J Neurosci 36:10356-10375
Truszkowski, Torrey L S; James, Eric J; Hasan, Mashfiq et al. (2016) Fragile X mental retardation protein knockdown in the developing Xenopus tadpole optic tectum results in enhanced feedforward inhibition and behavioral deficits. Neural Dev 11:14

Showing the most recent 10 out of 39 publications