The precise mechanism by which estrogen hormones influence brain feminization is not fully understood. According to some data, this process occurs during the prepubertal period. In our study, we divided female subjects into five groups. Four of them had their ovaries removed on the 10th day after birth, and from the 15th to the 25th day of age, we administered substances dissolved in corn oil that activate various estrogen hormone signaling pathways: 1) estradiol benzoate, 2) agonist of estrogen receptor α (ERα) propyl pyrazole triol, 3) agonist of estrogen receptor β - diarylpropiontril, 4) corn oil (negative control). For the fifth group (positive control), we used females that also received corn oil, but whose ovaries were removed after puberty (at 60 days of age). We evaluated feminization by observing female sexual behavior (lordosis), expression of tyrosine hydroxylase in the anteroventral part of the periventricular nucleus of the hypothalamus, and expression of ERα in the ventromedial nucleus of the hypothalamus. We found no statistically significant differences in lordosis or expression of these proteins in the brains of the different groups. Lordosis was weakly expressed in all groups, especially in the positive control. Our results suggest that activation of estrogen hormone signaling pathways had no lasting effects on the parameters we studied, and thus did not affect feminization. However, it is very likely that other factors influenced the results that may have disrupted the normal course of active feminization, particularly with respect to lordosis.