Prenatal and Neonatal Androgen Exposure Interact to Affect Sexual Differentiation in Female Rats

Rats were injected with oil on Days 17.5 and 18.5 of pregnancy or with 2 mg of testosterone propionate (TP) on Days 15.5 and 16.5, or Days 17.5 and 18.5, or Days 19.5 and 20.5. The female offspring were given oil or 5 μg of TP on Day 25 postconception. Among females exposed to TP only during prenata...

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Bibliographic Details
Published in:Behavioral neuroscience 1988-02, Vol.102 (1), p.61-65
Main Authors: Hoepfner, Bette Anne, Ward, Ingeborg L
Format: Article
Language:English
Subjects:
Animal
Animal Sexual Receptivity
Animals
Animals, Newborn
Biological and medical sciences
Estradiol - pharmacology
Estrus
Female
Female Animals
Fetus - drug effects
Fundamental and applied biological sciences. Psychology
Postnatal Period
Posture
Pregnancy
Prenatal Development
Progesterone - pharmacology
Rats
Rats, Inbred Strains
Reference Values
Sexual Behavior, Animal - drug effects
Sexual Development
Sexual differentiation and maturation. Puberty. Climacterium
Testosterone
Testosterone - pharmacology
Vertebrates: reproduction
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Summary:Rats were injected with oil on Days 17.5 and 18.5 of pregnancy or with 2 mg of testosterone propionate (TP) on Days 15.5 and 16.5, or Days 17.5 and 18.5, or Days 19.5 and 20.5. The female offspring were given oil or 5 μg of TP on Day 25 postconception. Among females exposed to TP only during prenatal ontogeny, a lower proportion of those treated on Days 17.5-18.5 of gestation displayed lordotic behavior than did the control group. Postnatal TP alone did not affect lordosis. However, all groups receiving combined pre- and postnatal TP showed impaired estrous patterns. The development of several components of morphology also was differentially affected by the timing of the androgen exposure. The data suggest that the differentiation of sexual behavior and reproductive morphology in the rat are influenced by an interaction of androgen dependent processes operating at different stages of perinatal ontogeny. Further, there may be an optimal fetal period during which androgenization sensitizes animals to low levels of testosterone circulating during neonatal development.
ISSN:0735-7044
1939-0084
DOI:10.1037/0735-7044.102.1.61