Oestrogen modulation of the effect of 8-OH-DPAT on prepulse inhibition: effects of aromatase deficiency and castration in mice.

[aromatase deficiency]

The aim of this study was to investigate the interaction of sex steroid hormones , particularly oestrogen , in the regulation of prepulse inhibition (PPI ) by serotonin-1 A (5 -HT 1 A ) receptors .We studied aromatase knockout (ArKO ) mice , which are unable to produce oestrogen but have high levels of testosterone , and the effects of castration .Treatment of male ArKO mice with the 5 -HT 1 A receptor agonist , 8 -hydroxy-dipropyl-aminotetralin (8 -OH -DPAT ), caused an increase in PPI that was significantly greater than in male wild-type controls . Castration of male mice caused a significant enhancement of the effect of 8 -OH -DPAT in control mice ; however , there was no change in the effect of this drug in ArKO mice . There was no significant effect of 8 -OH -DPAT on PPI in either female ArKO or wild-type controls . In all experiments , the effects of 8 -OH -DPAT on startle were not different between the groups . [3 H ]8 -OH -DPAT autoradiography showed no differences in 5 -HT 1 A receptor binding densities in areas of the forebrain , hippocampus or raphe region that could explain the PPI results . These data show that the absence of oestrogen in male ArKO mice leads to a greater effect of 5 -HT 1 A receptor stimulation on PPI . This effect can be mimicked in male control mice by castration . The differential involvement of oestrogen and testosterone in these animal models is discussed .

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Diseases presenting "areas of the forebrain" symptom

aromatase deficiency

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