Abstract

The overall focus of the research remains that of understanding the influences on neural development and later function that may be mediated via interactions at the level of membrane receptors. Many psychotherapeutic drugs act at this level. Research conducted in this laboratory has demonstrated pronounced effects on the noradrenergic (NE) innervation to the hypothalamus following in-utero exposure to diazepam (DZ), effects that are related to the binding of the drug to the central type benzodiazepine (BZ) receptor. Studies are now proposed to investigate the relationship between the BZ receptor and hypothalamic NE neurons and determine how these neurons are permanently influenced by the prenatal exposure. Specifically: (1) Do the effects on the NE neurons induced by the exposure involve changes in calcium uptake and/or (2) alterations in intracellular pools of NE in the hypothalamus? (3) What accounts for the apparent selectivity of the effect on hypothalamic NE neurons? Are a high percentage of BZ receptors in the hypothalamus presynaptically located on NE terminals in that region or is there a particular subtype of the central receptor in that region? Is the specificity of the in-utero exposure related to the relationship of hypothalamic NE-containing neurons to peptide-containing neurons, particularly those containing CRF and/or vasopressin? (4) What accounts for the delayed appearance of the effects induced by the prenatal exposure until after 4-5 weeks postnatal age? Are events related to puberty responsible? (5) Does DZ interaction with BZ receptors during fetal life influence the hypothalamic NE neurons at that time? Where in this region are the receptors located during the critical period for exposure? (6) Will physiologic stimuli such as restraint stress activate the BZ receptor during gestation and induce results similar to those observed following DZ exposure? Prenatal DZ exposure also induces alterations in the acoustic startle response and its potentiation by background noise, effects that appear unrelated to an influence at the central type receptor. Additionally, DZ administered to adult rats appear to inhibit the potentiated response via more than one mechanism. Continued analysis of this observation will assist in determining (1) whether there are different anxiolytic mechanisms and (2) whether prenatal DZ exposure influences the appearance of the different mechanisms. These studies will provide information on how DZ can influence the developing nervous system thereby yielding knowledge on neural interaction that can regulate development.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
2R01MH031850-07
Application #
3375263
Study Section
(BPNA)
Project Start
1979-07-01
Project End
1989-04-30
Budget Start
1986-05-01
Budget End
1987-04-30
Support Year
7
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Rochester
Department
Type
Schools of Arts and Sciences
DUNS #
208469486
City
Rochester
State
NY
Country
United States
Zip Code
14627

  Publications

Bitran, D; Purdy, R H; Kellogg, C K (1993) Anxiolytic effect of progesterone is associated with increases in cortical allopregnanolone and GABAA receptor function. Pharmacol Biochem Behav 45:423-8
Bitran, D; Primus, R J; Kellogg, C K (1991) Gestational exposure to diazepam increases sensitivity to convulsants that act at the GABA/benzodiazepine receptor complex. Eur J Pharmacol 196:223-31
Bitran, D; Hilvers, R J; Kellogg, C K (1991) Anxiolytic effects of 3 alpha-hydroxy-5 alpha[beta]-pregnan-20-one: endogenous metabolites of progesterone that are active at the GABAA receptor. Brain Res 561:157-61
Primus, R J; Kellogg, C K (1991) Experience influences environmental modulation of function at the benzodiazepine (BZD)/GABA receptor chloride channel complex. Brain Res 545:257-64
Bitran, D; Hilvers, R J; Kellogg, C K (1991) Ovarian endocrine status modulates the anxiolytic potency of diazepam and the efficacy of gamma-aminobutyric acid-benzodiazepine receptor-mediated chloride ion transport. Behav Neurosci 105:653-62
Kellogg, C K; Sullivan, A T; Bitran, D et al. (1991) Modulation of noise-potentiated acoustic startle via the benzodiazepine--gamma-aminobutyric acid receptor complex. Behav Neurosci 105:640-6
Primus, R J; Kellogg, C K (1991) Gonadal status and pubertal age influence the responsiveness of the benzodiazepine/GABA receptor complex to environmental challenge in male rats. Brain Res 561:299-306
Kellogg, C K; Primus, R J; Bitran, D (1991) Sexually dimorphic influence of prenatal exposure to diazepam on behavioral responses to environmental challenge and on gamma-aminobutyric acid (GABA)-stimulated chloride uptake in the brain. J Pharmacol Exp Ther 256:259-65
Miranda, R; Ceckler, T; Guillet, R et al. (1990) Early developmental exposure to benzodiazepine ligands alters brain 31P-NMR spectra in young adult rats. Brain Res 506:85-92
Primus, R J; Kellogg, C K (1990) Gonadal hormones during puberty organize environment-related social interaction in the male rat. Horm Behav 24:311-23

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