Abstract

The proposed research effort is designed to utilize multidisciplinary techniques in order to examine the hormonal regulation of peripheral autonomic neurons. In so doing these investigations will seek to answer a number of questions generated by testing the fundamental hypothesis that gonadal steroids exert regulatory influences on the growth and development of autonomic neurons and thus hormonal factors determine the biochemical and morphological characteristics of peripheral sympathetic neurons and parasympathetic neurons. The major questions to be answered include: 1) Do gonadal steroids influence both neurochemical (cholinergic and noradrenergic) and morphological (cell number, size, etc.) characteristics of ganglia? 2) Is there a critical time during which these hormonal factors are operative and do androgens and/or estrogens mediate these effects? 3) Do hormones exert their effects directly (i.e., are there androgen receptors in ganglia) or does testosterone regulate the target organ which in turn indirectly influences the neuron, or do both mechanisms exist? 4) Do hormonal factors regulate sympathetic maturation prenatally as well as postnatally. 5) Are similar regulatory influences operative in peripheral parasympathetic ganglia? This project will utilize well established biochemical, pharmacological, morphological, and microneurosurgical techniques in order to address the aforementioned hypothesis and questions. These pursuits will hopefully permit the development of new understandings of the manner and mechanisms by which endocrinological factors influence neuronal ontogeny, thus expanding our understanding of neuroendocrinological interactions during growth and development. Furthermore, such developmental studies may determine how prenatal and postnatal environmental factors alter ontogeny and result in developmental deficits. Accordingly, these experiments may bear upon birth defects secondary to perinatal injuries and pharmacological interactions and such specific developmental disorders as familial dysautono mia (Riley-Day Syndrome).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS022103-03
Application #
3404082
Study Section
Neurology C Study Section (NEUC)
Project Start
1986-12-01
Project End
1989-11-30
Budget Start
1988-12-01
Budget End
1989-11-30
Support Year
3
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of Rochester
Department
Type
School of Medicine & Dentistry
DUNS #
208469486
City
Rochester
State
NY
Country
United States
Zip Code
14627

  Publications

Goldstein, M E; Tank, A W; Fossom, L H et al. (1992) Molecular aspects of the regulation of tyrosine hydroxylase by testosterone. Brain Res Mol Brain Res 14:79-86
Romagnano, M A; Harshbarger, R J; Hamill, R W (1991) Brainstem enkephalinergic projections to spinal autonomic nuclei. J Neurosci 11:3539-55
Hamill, R W; Schroeder, B (1990) Hormonal regulation of adult sympathetic neurons: the effects of castration on neuropeptide Y, norepinephrine, and tyrosine hydroxylase activity. J Neurobiol 21:731-42
Melvin, J E; Hamill, R W (1989) Androgen-specific critical periods for the organization of the major pelvic ganglion. J Neurosci 9:736-42
Newton, B W; Romagnano, M A; Hamill, R W (1989) The ontogeny of substance P- and serotonin-like immunoreactivities in the sexually dimorphic cremaster nucleus of the rat spinal cord. Brain Res Dev Brain Res 47:227-42
Dail, W G; Hamill, R W (1989) Parasympathetic nerves in penile erectile tissue of the rat contain choline acetyltransferase. Brain Res 487:165-70
Romagnano, M A; Newton, B W; Pierre, A H et al. (1989) Postnatal ontogeny of enkephalin fibers in spinal sympathetic nuclei. Brain Res Dev Brain Res 46:263-79
Newton, B W; Hamill, R W (1988) Neuropeptide Y immunoreactivity is preferentially located in rat lumbar sexually dimorphic nuclei. Neurosci Lett 94:10-6
Melvin, J E; Hamill, R W (1987) The major pelvic ganglion: androgen control of postnatal development. J Neurosci 7:1607-12
Melvin, J E; Hamill, R W (1987) Altered sympathetic-salivary gland development: delayed response to postnatal castration. J Dent Res 66:751-5