Abstract
Interleukin-6 has been shown to cause imbalance between bone resorption and formation
in thyrotoxicosis. The aim of the present study was an attempt to estimate the influence
of estrogens on thyrotoxicosis-related disturbances in bone turnover in relation to
RANKL-RANK/osteoprotegerin system in IL-6 deficient mice. The study was performed
on 56, 12–13 weeks old, female mice: C57BL/6J (wild-type; WT) and C57BL/6JIL6–/–Kopf (IL-6 knock-out; IL6KO). The mice were randomly divided into 8 groups with 7 mice
in each one: 1. WT controls, 2. IL6KO controls, 3. WT mice with thyrotoxicosis, 4.
IL6KO mice with thyrotoxicosis, 5. WT ovariectomized, 6. IL6KO ovariectomized, 7.
WT ovariectomized mice with thyrotoxicosis, and 8. IL6KO ovariectomized mice with
thyrotoxicosis. Experimental model of menopause was evoked by bilateral ovariectomy
carried out in 8–9 weeks old mice. Thyrotoxicosis was induced by intraperitoneal injection
of levothyroxine at a dose of 1 μg/g daily over 21 days. The serum levels of TRACP5b,
osteocalcin, OPG, and RANKL were determined by ELISA. RANKL serum concentrations were
elevated significantly in all groups of ovariectomized mice as compared to respective
controls, however, in a minor degree in IL6KO thyrotoxic mice as compared to wild-type
animals. Osteoprotegerin serum levels were significantly increased in all thyrotoxic
groups of mice except ovariectomized IL6KO animals. To sum up, the results of the
present study suggest that IL-6 plays a key role in stimulation of RANKL-RANK/OPG
system and this effect is strongly enhanced in conditions of accelerated bone turnover
such as thyrotoxicosis and/or estrogen depletion.
Key words
sRANKL - OPG - IL-6 - hyperthyrosis - osteoporosis - IL-6 knock-out mice
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Correspondence
J. MysliwiecMD, PhD
Department of Endocrinology
Diabetology and Internal
Diseases
Medical University of Bialystok
M.C. Sklodowskiej-Curie 24 A
15-276 Bialystok
Poland
Phone: +48/85/746 82 39
Fax: +48/85/744 76 11
Email: janusz.mysliwiec@umwb.edu.pl