Abstract

This application proposes to evaluate a series of novel steroid chemical delivery systems which we have shown are selectively """"""""locked-into"""""""" the central nervous system (CNS). The proposed selective CNS delivery of gonadal steroids is based upon the chemical attachment of estradiol of testosterone to the lipid soluble dihydropyridine carrier. This steroid-carrier system readily crosses the blood brain barrier (BBB) and the carrier is rapidly oxidized to the corresponding hydrophilic pyridinium salt, thus reducing its rate of egress from the CNS. The hydrolysis of the steroid from its carrier results in the sustain release of the steroid in the brain and the rapid clearance of the non-toxic carrier. Preliminary evaluations of one estradiol-chemical delivery system (E2 -CDS) resulted in a dose-dependent sustained suppression of LH in female rats and in male rats a chronic (at least 24 days) suppression of LH release following a single injection. In the present application, we proposed to evaluate both the testosterone-chemical delivery system (T-CDS) and E2- CDS for the dose-dependency and time-course of suppression LH and FSH secretion, and the corresponding levels of released testosterone or E2 in the brain and peripheral tissue. With the identification of the optimal doses and sampling times, we will assess the mechanism of action of the steroid-CDS in chronically suppressing gonadotropin release by assessing the activity of neurons which contain luteinizing hormone-releasing hormone- releasing hormone (LHRH), by determining the responsiveness of anterior pituitary gonadotrophs to LHRH, and by assessing parameters of this pulsatile release of LH. We will evaluate the capacity of brain-specific delivery of gonadal steroids to reduced endogenous steroid secretion from the ovaries and/or testes. Finally, we will evaluate the E2-CDS and the T-CDS for their efficacy in reducing the rate of growth of endometrial and prostatic tissue in animal models for endometriosis and prostatic cancer. The proposed evaluations may lead to (i) a useful tool for dissociating central from peripheral effects of gonadal steroids, (ii) a selective treatment of brain estradiol deficiencies in women with vasomotor symptoms and (iii) the selective reduction in gonadotropin secretion for fertility regulation and the treatment of peripheral steroid-dependent diseases, such as prostatic hypertrophy or cancer, as well as endometriosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD022540-02
Application #
3322183
Study Section
Reproductive Endocrinology Study Section (REN)
Project Start
1987-08-01
Project End
1990-07-31
Budget Start
1988-08-01
Budget End
1989-07-31
Support Year
2
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of Florida
Department
Type
Schools of Pharmacy
DUNS #
073130411
City
Gainesville
State
FL
Country
United States
Zip Code
32611

  Publications

Rahimy, M H; Bodor, N; Simpkins, J W (1993) Suppression of plasma testosterone and prostate carcinoma size by a redox-based, brain-targeted estrogen delivery system in the rat. Prostate 23:79-90
Ganesan, R; Simpkins, J W (1991) Conditioned taste aversion induced by estradiol pellets. Physiol Behav 50:849-52
Rahimy, M H; Simpkins, J W; Bodor, N (1990) Dose and time-course evaluation of a redox-based estradiol-chemical delivery system for the brain. I. Tissue distribution. Pharm Res 7:1061-7
Ganesan, R; Simpkins, J W (1990) The role of conditioned taste aversion in the suppression of food intake by estradiol. Physiol Behav 48:647-52
Rahimy, M H; Simpkins, J W; Bodor, N (1990) Tissue distribution of a brain-enhanced chemical delivery system for estradiol. Drug Des Deliv 6:29-40
Ratka, A; Simpkins, J W (1990) Dose-dependent effects of chronic treatment with estradiol or progesterone on LH secretion in ovariectomized rats. Endocr Res 16:165-84
Millard, W J; Romano, T M; Bodor, N et al. (1990) Growth hormone (GH) secretory dynamics in animals administered estradiol utilizing a chemical delivery system. Pharm Res 7:1011-8
Rahimy, M H; Simpkins, J W; Bodor, N (1990) Dose and time-course evaluation of a redox-based estradiol-chemical delivery system for the brain. II. Pharmacodynamic responses. Pharm Res 7:1107-12
Anderson, W R; Simpkins, J W; Brewster, M E et al. (1989) Evidence for prolonged suppression of stress-induced release of adrenocorticotropic hormone and corticosterone with a brain-enhanced dexamethasone-redox delivery system. Neuroendocrinology 50:9-16
Rahimy, M H; Bodor, N; Simpkins, J W (1989) A rapid, sensitive method for the simultaneous quantitation of estradiol and estradiol conjugates in a variety of tissues: assay development and evaluation of the distribution of a brain-enhanced estradiol-chemical delivery system. J Steroid Biochem 33:179-87

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