Pharmacologic inhibition of particulate-induced bone resorption

Abstract

In this study, a rat calvaria/macrophage co-culture model was used to study the effects of various agents upon bone resorption induced by macrophage exposure to bone cement particles. The experimental group consisted of calvaria bone disks set in tissue culture medium on stainless-steel platforms into wells with macrophages adherent to the bottom which are exposed to the particles. Tumor necrosis factor α (TNF-α), prostaglandin E₂ (PGE₂), and calcium 45 (Ca⁴⁵) were released in significant amounts in this system. Interleukin 1α (IL-1α) was not detected. Indomethacin inhibited the production of PGE₂, but did not affect TNF release or inhibit the release of Ca⁴⁵. Anti-TNF antibody neutralized the presence of TNF to undetectable levels, but did not affect PGE₂ release or inhibit Ca⁴⁵ release. The addition of calcitonin did not inhibit Ca⁴⁵ release by calvaria. In contrast, the addition of disodium pamidronate, a member of the bisphosphonate family, was effective in inhibiting the release of Ca⁴⁵ even after 96 h of incubation. In prior studies, incubation of calvaria in conditioned medium from macrophages exposed to cement particles led to resorption through a mechanism which is dependent upon TNF production by macrophages, and PGE₂ production by cells in bone. In this two-way system, in which macrophages and cells in bone are allowed to interact, this dependency was no longer evident. Pamidronate was the only agent tested which suppressed the increase in bone resorption associated with macrophage exposure to bone cement particles to levels which were not significantly different from unexposed calvaria. By delaying or preventing bone resorption associated with macrophage exposure to bone cement particles, bisphosphonates may have a clinical role in cemented joint arthroplasty by decreasing the rate or incidence of aseptic loosening and prolonging implant longevity. © 1996 John Wiley & Sons, Inc.