Study of normal prostate organogenesis and the effects of intrauterine and pubertal androgenic exposure on the morphophysiology of old gerbil prostate

Recent researches have been shown that the predisposition to prostatic disorders has its origin during moments of early life. Therefore, the detailed understanding of prostate organogenesis and the mechanisms underlying in predisposing to these disorders are extremely important in order to highlight the etiology of prostatic pathologies. Thus, the aim of this work was to evaluate the normal prostate organogenesis and the influence of testosterone exposure during prenatal and pubertal life on the prostate of male and female Mongolian gerbil. To this, the present work was divided into two phases. First, groups of pregnant female received subcutaneous injections of testosterone (500 µg/dosage) four days before the parturition (groups TG and TG + T) and/or during postnatal life (groups C + T and TG + T). The offspring of these mothers aged, being killed with one-year-old. In a second moment, we realized a normative study of the organogenesis of male ventral prostate lobe. To this, male fetus with 20 and 24 (E20 - E24) days of gestation, besides newborn with one-day-old (P1), were employed in this study. All tissue fragments were dissected and fixed in methacarn or 4% paraformaldehyde, being processed for paraffin embedding. Following, tissue sections were submitted to biometrical, morphological, stereological, immunohistochemical, immunofluorescence and three dimensional reconstruction analyses. The results showed that only the old males of TG + T group were affected by adenomatous hyperplasia associated with inflammation, although in other male experimental groups we also observed hyperplastic foci in the prostate. The female exposed to testosterone during prenatal phase (TG and TG + groups) have demonstrated a higher heterogeneity of alterations due treatment, being characterized by reproductive system malformations, formation of ectopic prostatic tissue surrounding vaginal wall, besides the presence of prostatic lesions characterized by adenomatous hyperplasic foci. These findings show that abnormal prenatal exposure to testosterone affect the prostate morphogenesis in both male and female, disrupting normal developmental processes and increasing the susceptibility to the development of prostatic diseases during aging. Regarding the prostate organogenesis study, it was observed that the first ventral buds emerge from the ventral urethral epithelium between the 20th and 21th day of prenatal life, reaching the ventral mesenchymal pad (VMP) and initiating the branching process at the first day of postnatal life. We also noted that the smooth muscle layer seems to have a central play during this process, which may act as physical barrier to the buds heading to VMP. Regarding the nuclear receptors, the androgen presented a high immunomarking at the periurethral mesenchyme, whereas cells with positive marking for estrogen receptor alpha were identified either in the periurethral mesenchyme or in the buds. Finally, the results demonstrate that the prostate organogenesis, besides involving a series of events finely regulated, is an extremely sensitive and crucial to the health of the gland throughout the life (AU)