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Abstract
The localization of androgen receptors (AR) and their
ligands in the uterine microenvironment at early pregnancy
suggest a role for AR in uterine physiology. We have
evaluated AR expression in the pig uterine endometrium and
examined whether AR ligands modulate peri-implantation
uterine gene expression. Northern blot analysis
demonstrated the ~10.5 Kb AR transcript in endometrium.
Endometrial levels of AR mRNA and protein were greater at
early- than at mid- or late-pregnancy. Estrogen
receptor-
mRNA levels showed similar maximal
expression at early pregnancy. Immunocytochemical
analysis of endometrium at early pregnancy localized AR to
nuclei of glandular epithelial (GE) and stromal (ST)
cells. To evaluate a role for AR in uterine gene
regulation, the levels of mRNAs for insulin-like growth
factor-I (IGF-I), proliferative cell nuclear antigen
(PCNA), and AR itself, were assessed in uterine
endometrial explant cultures treated with
17
-estradiol (E), testosterone (T), and
19-nortestosterone (N). Induction by E of AR mRNA
abundance occurred in endometrium from day 10, but not
from day 12 pregnant animals and this was partially
blocked by co-addition of N or T, although neither
androgen alone had any effect. Abundance of IGF-I and
PCNA mRNAs was increased by E and inhibited by co-addition
of either T or N in day 10 pregnant pig endometrium. In
endometrium from day 12 pregnant animals, addition of
either N or T with E increased IGF-I mRNA levels over that
of controls, although E alone was without effect. In
contrast, PCNA mRNA abundance was suppressed by all
steroid treatments in these explants. DNA synthesis in
primary cultures of GE cells from endometrium at days 10
and 12 of pregnancy was increased by E and was suppressed
by T, the latter only at day 12. E did not affect DNA
synthesis in ST cells from endometrium at either pregnancy
day, although T inhibited this process in an E-dependent
manner in ST cells from pregnancy day 12. Results
identify AR in the pig endometrium during the window of
maternal receptivity for implantation, and demonstrate the
functional, albeit complex, interactions of androgens and
estrogens in the regulation of uterine endometrial gene
expression and cell growth in vitro. Further
elucidation of the role of androgens and their receptor in
early pregnancy events may be relevant to an understanding
of peri-implantation embryo loss.
Key words:
Embryo
Pregnancy
Androgen receptor
Estradiol receptor
Uterus
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