Medial Preoptic Area, Estrogen, and the Peripubertal Desensitization to the Negative Estrogen Feedback in Female Rats

Döcke, F; Rohde, Wolfgang; Gerber, Peter Arne; Kreuz, Gerold

doi:10.1159/000123959

Cited by 12 publications

(15 citation statements)

References 21 publications

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“…Former studies [10][11][12] had shown that the sensitivity to the gonadotrophin, particularly the LH-inhibiting effect of estrogen, declines substantially in immature and cyclic female rats prior to the onset of puberty and during the preovulatory phase of the ovarian cycle, respectively. The desensitization of the negative estrogen feedback is proba bly induced by increasing estrogen levels in the blood [11,13], and preliminary results [16] suggested that inhibition of the medial preoptic DA activity might be involved.…”

Section: Discussionmentioning

confidence: 99%

“…The desensitization of the negative estrogen feedback is proba bly induced by increasing estrogen levels in the blood [11,13], and preliminary results [16] suggested that inhibition of the medial preoptic DA activity might be involved. The relationship between this activity and the sensitivity of the negative estrogen feedback was investigated in the present study.…”

Section: Discussionmentioning

confidence: 99%

“…This mechanism may essentially be involved in the control of female puberty and of the ova rian cycle [10,II,13]. The present findings suggest a possi ble relationship between the desensitization to the gonado trophin-inhibiting effect of estrogen and the medial preop tic DA neurotransmission, because (1) high DA activity in the MPOA enhanced, whereas low activity diminished, the inhibition of LH secretion by EB; (2) alteration of this acti vity markedly affected the onset of puberty and ovarian cy clicity, and (3) preliminary evidence was obtained sugges ting an inhibitory effect on the DA transmission in the MPOA of an estrogen treatment that induced desensitiza tion of the negative estrogen feedback.…”

Section: Discussionmentioning

confidence: 99%

“…Similar implants located in the VMAR were ineffective in this regard. The results suggest that: (1) low DA activity in the M POA reduces and high activity enhances the sensitivity of the negative estrogen feedback in immature and adult female rats; (2) the medial preoptic DA activity seems to be involved in the control of female puberty and of the ovarian cycle, and (3) a relationship may exist between the estrogen-induced prepu bertal and preovulatory desensitization of the negative estrogen feedback and the DA neurotransmission in the MPOA.Recent studies in female rats demonstrated that the sen sitivity to the gonadotrophin-inhibiting effect of estrogen declines prepubertally and during the preovulatory phase of the ovarian cycle [10][11][12]. Further results suggested that estrogen itself induces the desensitization process by an in hibitory action on the medial preoptic area (MPOA), be cause both the local implantation of very low amounts of estradiol benzoate (EB) and bilateral lesioning of this region diminished considerably the inhibition of gonado trophin secretion by estrogen in immature and adult rats [ 11,13].…”

mentioning

confidence: 99%

“…Further results suggested that estrogen itself induces the desensitization process by an in hibitory action on the medial preoptic area (MPOA), be cause both the local implantation of very low amounts of estradiol benzoate (EB) and bilateral lesioning of this region diminished considerably the inhibition of gonado trophin secretion by estrogen in immature and adult rats [ 11,13].…”

mentioning

confidence: 99%

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Influence of the Medial Preoptic Dopaminergic Activity on the Efficiency of the Negative Estrogen Feedback in Prepubertal and Cyclic Female Rats

et al. 1987

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Immature and adult female rats were bilaterally implanted in the medial preoptic area (MPOA) or hypothalamic ventromedial-arcuate region (VMAR) with the dopamine (DA) antagonist, pimozide, or the DA agonist, apomor-phine, and the sensitivity to the LH-inhibiting effect of a subcutaneous injection of estradiol benzoate (EB), the onset of puberty and ovarian cyclicity were investigated. Diminution of the inhibitory effect of EB on LH secretion was recorded in ovariectomized immature and adult females implanted in the MPOA with pimozide. This response was not obtained in rats implanted in the VMAR. In contrast, medial preoptic, but not intrahypothalamic, implantation of agar pellets containing apomorphine resulted in enhanced sensitivity to estrogen both prepubertally and during the ovarian cycle. The sensitizing effect of apomorphine was completely prevented in prepubertal rats by pretreatment with EB for 6 days. Bilateral implantation of pimozide-agar pellets in the MPOA of 28-day-old intact females induced significant advancement of the onset of puberty, whereas sexual maturation was not affected by daily subcutaneous injections of the DA antagonist from day 28 till the day of vaginal opening. In adult 4-day-cyclic rats fitted with guide cannulae, the forthcoming ovulation was delayed for about 7 days as compared to the controls implanted with agar if apomorphine was placed in the MPOA from the morning of metestrus to the morning of diestrus. Similar implants located in the VMAR were ineffective in this regard. The results suggest that: (1) low DA activity in the MPOA reduces and high activity enhances the sensitivity of the negative estrogen feedback in immature and adult female rats; (2) the medial preoptic DA activity seems to be involved in the control of female puberty and of the ovarian cycle, and (3) a relationship may exist between the estrogen-induced prepubertal and preovulatory desensitization of the negative estrogen feedback and the DA neurotransmission in the MPOA.

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