Calcitonin-like effects of forskolin and choleratoxin on surface area and motility of isolated rabbit osteoclasts
Open Access
- 1 December 1988
- journal article
- research article
- Published by Oxford University Press (OUP) in Journal of Bone and Mineral Research
- Vol. 3 (6) , 611-619
- https://doi.org/10.1002/jbmr.5650030606
Abstract
We have previously found that the adenylate cyclase stimulators forskolin and choleratoxin increase cyclic AMP and transiently inhibit bone resorption in cultured mouse calvaria, suggesting that the compounds, directly or indirectly, may inhibit osteoclast activity. In the present study, forskolin and choleratoxin were investigated for their direct effects on surface area and motility of isolated rabbit osteoclasts, and the effects were compared to those of calcitonin (CT). Osteoclasts were cultured on coverslips for different times in the absence or presence of the compounds. The effect on osteoclast mean area was quantified on fixed and stained osteoclasts, and in addition effects were recorded with time-lapse cinemicrography. The effects of CT (100 mU/ml) on mean area and motility were seen within minutes and were maximal after 10–60 minutes. Forskolin (10–30 μmol/liter) produced a rapid (15–60 minutes) inhibition of motility and decrease in area (contraction) of osteoclasts. Choleratoxin (1 μg/ml) treatment also resulted in cell contraction and inhibition of motility; however, the response was not seen before 45–60 minutes. The difference in the kinetics of the osteoclast response between forskolin, CT, and choleratoxin is similar to differences in time course for the effect on cyclic AMP in calvarial bones, which we reported earlier. Although cells were incubated continuously with forskolin, choleratoxin, or CT, the effects were transient. Thus, after 7–8 h incubation with CT, 3–4 h treatment with forskolin, or 4–6 h with choleratoxin, the osteoclasts started to recover from contraction and immotility. The effect of forskolin and choleratoxin on the mean surface area of osteoclasts was dose dependent. The present study shows that forskolin and choleratoxin have a direct inhibitory action on osteoclast activity and thus provide further evidence that cyclic AMP is a mediator of the action of CT on bone resorption.Keywords
Funding Information
- Faculty of Dentistry
- Swedish Medical Research Council ((B 86-24X-07525))
This publication has 29 references indexed in Scilit:
- Effects of cholera toxin on cyclic AMP accumulation and bone resorption in cultured mouse calvariaBiochimica et Biophysica Acta (BBA) - Molecular Cell Research, 1987
- Forskolin has both stimulatory and inhibitory effects on bone resorption in fetal rat long bone culturesJournal of Bone and Mineral Research, 1986
- Actions of calcitonin, parathyroid hormone, and prostaglandin E2 on cyclic AMP formation in chicken and rat osteoclastsJournal of Cellular Biochemistry, 1986
- A two-receptor model for the action of parathyroid hormone on osteoblasts: A role for intracellular free calcium and cAMPCell Calcium, 1985
- Transient inhibition on calcium mobilization from cultured mouse calvarial bones by the adenylate cyclase stimulator forskolinActa Physiologica Scandinavica, 1984
- Inhibition of Bone Resorption and Increased Incorporation of 3H-Glucosamine into Hyaluronate in Bone Organ Cultures Treated with Dibutyryl Cyclic AMP and ColchicinePathobiology, 1983
- Calcitonin alters behaviour of isolated osteoclastsThe Journal of Pathology, 1982
- Stimulation of bone resorption in organ culture by cholera toxinBiochemical and Biophysical Research Communications, 1981
- Comparison of Inhibition of Bone Resorption and Escape with Calcitonin and Dibutyryl 3′, 5′ Cyclic Adenosine MonophosphateEndocrine Research Communications, 1981
- Inhibition by cholera toxin of parathyroid hormone-induced calcium release from bone in cultureBiochemical and Biophysical Research Communications, 1977