Introduction: osteoporosis is characterized by low bone mass and density, as well as change in microarchitecture of bone tissue leading to
decreased bone strength. In vitro research shows nicotine can increase osteoblast activity and proliferation, also suppress osteoclast activity.
Therefore we explore nicotine anti-resorptive property by in vivo true experimental and randomized posttest only controlled group research that was
conducted in 18-20 weeks old Rattus norvegicus. Methods: twenty-five female rats were divided into five groups, with 5 rats per group. The first
group represented normal rats (Sham), while the second to fifth group underwent bilateral ovariectomy. The second group serves as positive control
group (ovariectomy-only/OVX). The third to fifth group serve as dose 1 (P1-0.25mg/kg), dose 2 (P2-0.5 mg/kg), and Dose 3 (P3-0.75 mg/kg)
treatment group receiving daily per-oral nicotine for 28 days, started 3 weeks post- ovariectomy. After 28 days treatment, the serum was checked.
Results: nicotine has dose-dependent manner on serum osteocalcin and serum DPD level. Level of osteocalcin in P2 group was significantly lower
(Mann-Whitney, p = 0.008) compared to OVX group (59.4% lower). Level of DPD in all group was not significantly different (ANOVA, p < 0.05) but
shows lowest level in P2 group. For serum calcitonin level, there's no significant different between groups. Conclusion: nicotine at right low-dose
might be able to inhibit osteoclast activity, thus open a possibility of anti-resorptive property of nicotine.