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Department of Orthopedic Research (J.D.S., H.D., R.M.H., R.T.T.) and Biochemistry and Molecular Biology (R.T.T.), Mayo Clinic, Rochester, Minnessota 55905
Address all correspondence and requests for reprints to: Russell T. Turner, Ph.D., Mayo Clinic, Department of Orthopedics, Medical Science Building 369, 200 First Street SW, Rochester, Minnesota 55905. E-mail: rolbiecki.lori{at}mayo.edu
We examined the specificity of the steroidal antiestrogen ICI 182,780
(ICI) on bone and reproductive tissues in adult and growing female
rats. Using a 1.5-mg/kg dose (sc), we evaluated the effects of ICI on
the bone, body weight, uterine weight, serum cholesterol, and serum
estradiol in either adult and/or growing rats. ICI increased serum
estradiol cholesterol in ovary-intact rats, had no effect on uterine
weight in ovariectomized rats, and resulted in uterine atrophy in
ovary-intact animals comparable with ovariectomy. In contrast, ICI had
no effect on body weight. In bone, ICI significantly increased the rate
of periosteal bone formation in long bones of growing and mature female
rats. In contrast, ICI had no effect on longitudinal bone growth in
rapidly growing rats. When ICI was administered to mature rats with or
without ovaries, two-factor ANOVA revealed significant interaction
(P
0.05) between ovariectomy and ICI treatment
for cancellous bone area and labeled bone perimeter. ICI increased
skeletal indices of bone turnover in the cancellous bone of
ovary-intact rats but reduced these indices of bone turnover in the
cancellous bone of ovariectomized rats. The increase in bone turnover
was associated with a reduction in cancellous bone area in the
ovary-intact rats. A reduction in bone turnover was similarly
associated with an increase in bone area in the ICI-treated
ovariectomized rats. In summary, ICI exhibited complete estrogen
antagonism in cortical and cancellous bone, partial agonism in
cancellous bone, and no activity on tibial longitudinal growth rate of
growing ovary-intact rats. The effects in adult rats were influenced by
circulating levels of estradiol. ICI had no activity on body weight and
complete antagonism on uterine weight. These results demonstrate that a
ligand with high binding affinity to the estrogen receptor(s) can
elicit an array of estrogen-mediated regulation of bone metabolism.
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