Abstract

Neurons are normally overproduced and subsequently die in early development. We propose to investigate this overproduction and death in the mammalian retina, midbrain and visual cortex, to determine what factors contribute to a neuron's survival. In a midbrain structure, the superior colliculus, we will manipulate the amount of afference and determine both the range over which synaptic density may vary and the relationship of synaptic density to cell death. In the retain, we will determine if the day a neuron is generated can predict the likelihood and timing of its death, using thymidine autoradiography. For the visual cortex, we will determine if its cellular laminae respond to input and target deletions in the same way other neural structures have been shown to, with the goal of determining how local variations in morphology and cell number are imposed on the general neocortical plan. Finally, we will relate the timing of establishment of connections to and from these structures to the pattern of cell death. In all cases, we will be quantifying the amount of observable cellular degeneration in early brain development consequent to our manipulations. In sum, we propose to investigate the early control of a neuron's survival and also use the information about the patterns of early neuron death to inform us about the mechanisms of the establishment of orderly connections in the developing mammalian brain. This work will have direct relevance for our understanding of the nature of, and the reasons for, reorganization of the human brain following perinatal damage.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Modified Research Career Development Award (K04)
Project #
5K04NS000783-05
Application #
3074688
Study Section
Visual Sciences B Study Section (VISB)
Project Start
1983-07-01
Project End
1988-06-30
Budget Start
1987-07-01
Budget End
1988-06-30
Support Year
5
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Cornell University
Department
Type
Schools of Arts and Sciences
DUNS #
City
Ithaca
State
NY
Country
United States
Zip Code
14850

  Publications

Xiong, M; Finlay, B L (1993) Changes in synaptic density after developmental compression or expansion of retinal input to the superior colliculus. J Comp Neurol 330:455-63
Miller, B; Windrem, M S; Finlay, B L (1991) Thalamic ablations and neocortical development: alterations in thalamic and callosal connectivity. Cereb Cortex 1:241-61
Windrem, M S; Finlay, B L (1991) Thalamic ablations and neocortical development: alterations of cortical cytoarchitecture and cell number. Cereb Cortex 1:230-40
Pallas, S L; Finlay, B L (1989) Conservation of receptive-field properties of superior colliculus cells after developmental rearrangements of retinal input. Vis Neurosci 2:121-35
Kelling, S T; Sengelaub, D R; Wikler, K C et al. (1989) Differential elasticity of the immature retina: a contribution to the development of the area centralis? Vis Neurosci 2:117-20
Finlay, B L; Pallas, S L (1989) Control of cell number in the developing mammalian visual system. Prog Neurobiol 32:207-34
Wikler, K C; Perez, G; Finlay, B L (1989) Duration of retinogenesis: its relationship to retinal organization in two cricetine rodents. J Comp Neurol 285:157-76
Henderson, Z; Finlay, B L; Wikler, K C (1988) Development of ganglion cell topography in ferret retina. J Neurosci 8:1194-205
Windrem, M S; Jan de Beur, S; Finlay, B L (1988) Control of cell number in the developing neocortex. II. Effects of corpus callosum section. Brain Res 471:13-22
Pallas, S L; Gilmour, S M; Finlay, B L (1988) Control of cell number in the developing neocortex. I. Effects of early tectal ablation. Brain Res 471:1-11

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