Abstract

Our long term objective is to prevent human BPH (benign prostatic hyperplasia) or to improve the clinical course of individuals suffering from it. The present application was proposed with the assumption that the canine prostate is an acceptable model for studying the pathogenesis of human BPH and with the hypothesis that systemic, primarily hormonal, factors other than androgen are required in the canine BPH pathogenesis. The present application postulates that two sources of these critical non-androgenic humoral factors warrant consideration: PITUITARY and TESTIS. The testis, besides secreting testosterone, is known to produce a large variety of substances. Among them are estrogen, androgen binding protein, transferrin, inhibin, Mullerian inhibiting substance, etc. The cells responsible for the production of these substances are Sertoli cells. Results of our initial experiments summarized in this report indicate a role for the testes in the maintenance of BPH in old dogs and experimental induction of BPH in young dogs. The serum and prostatic tissue hormone levels noted in these experiments support the concept that the systemic factor(s) responsible for this role is a non-androgenic secretory product. The pituitary secretes hormones having direct effects on the testis which, in turn, stimulates prostatic growth and function. In addition, these hormones and others (e.g. prolactin) may act synergistically with androgen to promote prostatic growth and possibly to induce and promote BPH development. Therefore, the objectives for the present proposal are two-fold. First, we propose to conduct both in vivo and in vitro experiments in an attempt to demonstrate a direct effect of pituitary secretions on the canine prostate. Second, in vitro experiments will be conducted to study the effects of Sertoli cell secretions on the canine prostate. Specifically, the following experiments will be conducted: (1) Hypophysectomy and castration in experimental dogs and evaluate the effect of estrogen-androgen synergism on canine prostate, (2) pituitary grafting under the renal capsule and study the castration-induced regression and androgen-stimulated growth of the canine prostate, (3) establish organ culture system for the canine prostate and to study the direct effect of various non- androgenic substances, and (4) to establish tissue culture systems of the canine Sertoli cells and to use the Sertoli cell spent media for qualitative protein analysis (two-dimensional electrophoresis) and to cultivate the canine prostate.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Specialized Center (P50)
Project #
5P50DK039250-05
Application #
3855101
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
5
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Northwestern University at Chicago
Department
Type
DUNS #
005436803
City
Chicago
State
IL
Country
United States
Zip Code
60611

  Publications

Ilio, K Y; Nemeth, J A; Sensibar, J A et al. (2000) Prostatic ductal system in rats: changes in regional distribution of extracellular matrix proteins during castration-induced regression. Prostate 43:10-Mar
Kassen, A E; Sensibar, J A; Sintich, S M et al. (2000) Autocrine effect of DHT on FGF signaling and cell proliferation in LNCaP cells: role of heparin/heparan-degrading enzymes. Prostate 44:124-32
Sensibar, J A; Pruden, S J; Kasjanski, R Z et al. (1999) Differential growth rates in stromal cultures of human prostate derived from patients of varying ages. Prostate 38:110-7
Lee, C; Sintich, S M; Mathews, E P et al. (1999) Transforming growth factor-beta in benign and malignant prostate. Prostate 39:285-90
Kim, I Y; Ahn, H J; Lang, S et al. (1998) Loss of expression of transforming growth factor-beta receptors is associated with poor prognosis in prostate cancer patients. Clin Cancer Res 4:1625-30
Kim, I Y; Zelner, D J; Lee, C (1998) The conventional transforming growth factor-beta (TGF-beta) receptor type I is not required for TGF-beta 1 signaling in a human prostate cancer cell line, LNCaP. Exp Cell Res 241:151-60
Grayhack, J T; Kozlowski, J M; Lee, C (1998) The pathogenesis of benign prostatic hyperplasia: a proposed hypothesis and critical evaluation. J Urol 160:2375-80
Sherwood, E R; Van Dongen, J L; Wood, C G et al. (1998) Epidermal growth factor receptor activation in androgen-independent but not androgen-stimulated growth of human prostatic carcinoma cells. Br J Cancer 77:855-61
Grayhack, J T; Sensibar, J A; Ilio, K Y et al. (1998) Synergistic action of steroids and spermatocele fluid on in vitro proliferation of prostate stroma. J Urol 159:2202-9
Gann, P H; Chatterton, R; Vogelsong, K et al. (1997) Epidermal growth factor-related peptides in human prostatic fluid: sources of variability in assay results. Prostate 32:234-40

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