Bisphosphonates: molecular mechanisms of action and effects on bone cells, monocytes and macrophages

Anke J Roelofs, Keith Thompson, Frank Ebetino, Michael J Rogers, Fraser Coxon

Research output: Contribution to journalReview article

121 Citations (Scopus)

Abstract

Bisphosphonates are widely used in the treatment of diseases involving excessive bone resorption, such as osteoporosis, cancer-associated bone disease, and Paget’s disease of bone. They target to the skeleton due to their calcium-chelating properties, where they primarily act by inhibiting osteoclast-mediated bone resorption. The simple bisphosphonates, clodronate, etidronate and tiludronate, are intracellularly metabolised to cytotoxic ATP analogues, while the more potent, nitrogen-containing bisphosphonates act by inhibiting the enzyme FPP synthase, thereby preventing the prenylation of small GTPases that are necessary for the normal function and survival of osteoclasts. In recent years, these concepts have been refined, with an increased understanding of the exact mode of inhibition of FPP synthase and the consequences of inhibiting this enzyme. Recent studies further suggest that the R2 side chain, as well as determining the potency for inhibiting the target enzyme FPP synthase, also influences bone mineral binding, which may influence distribution within bone and duration of action. While bisphosphonates primarily affect the function of resorbing osteoclasts, it is becoming increasingly clear that bisphosphonates may also target the osteocyte network and prevent osteocyte apoptosis, which could contribute to their anti-fracture effects. Furthermore, increasing evidence implicates monocytes and macrophages as direct targets of bisphosphonate action, which may explain the acute phase response and the anti-tumour activity in certain animal models. Bone mineral affinity is likely to influence the extent of any such effects of these agents on non-osteoclast cells.
Original languageEnglish
Pages (from-to)2950-2960
Number of pages11
JournalCurrent Pharmaceutical Design
Volume16
Issue number27
DOIs
Publication statusPublished - Sep 2010

Keywords

  • bisphosphonate
  • FPP synthase
  • protein prenylation
  • bone affinity
  • osteoclast
  • osteocyte
  • monocyte
  • macrophage
  • bisphosphonates
  • Paget's disease
  • clodronate
  • etidronate
  • tiludronate
  • anti-tumour activity
  • non-osteoclast cells
  • post-menopausal osteoporosis
  • hypercalcaemia of malignancy
  • risedronate
  • zoledronate
  • minodronate
  • mitochondrial adenine nucleotide translocase (ANT)
  • mevalonate pathway
  • cholesterol biosynthetic pathway
  • nitrogen-bisphosphonates
  • biosynthetic pathway
  • mevalonate-to-cholesterol
  • oral bioavailability
  • binding affinity
  • technetium-99m conjugates
  • osteoclasts
  • potent inhibitory effects
  • n-bisphosphonates
  • alendronate therapy
  • putative effects
  • bisphosphonate therapy
  • monocyte-macrophage lineage
  • anti-inflammatory effects
  • antigen-presenting cells
  • tumour-associatied macrophages
  • haematological malignancies
  • anti-tumour effects
  • anti-tumorlal phe-notype

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