Osteogenic inhibition by rat periodontal ligament cells: modulation of bone morphogenic protein-7 activity in vivo |
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| Authors: | Dhaarmini Rajshankar Christopher A G McCulloch Howard C Tenenbaum P C Lekic |
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| Institution: | (1) Samuel Lunenfeld Research Institute, Mount Sinai Hospital, Toronto, Canada, CA;(2) MRC Group in Periodontal Physiology, Faculty of Dentistry, University of Toronto, Canada, CA;(3) Faculty of Dentistry, University of Manitoba, 780 Bannatyne Avenue, Winnipeg, Manitoba, R3E 0W2, Canada Tel.: +1 204 789 3507; Fax: +1 204 789 3913, CA |
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| Abstract: | Periodontal ligament width is precisely maintained throughout the lifetime of adult mammals but the biological mechanisms
that inhibit ingrowth of bone into this soft connective tissue are unknown. As bone morphogenic proteins strongly stimulate
osteogenesis and can induce ectopic bone formation in vivo, we tested the hypothesis that topical application of this powerful
osteogenic agent will overwhelm the osteogenic inhibitory mechanisms of periodontal ligament cells and induce ankylosis. Wounds
through the alveolar bone and periodontal ligament were created in 45 male Wistar rats. Defects were filled with either a
collagen implant or collagen plus bone morphogenic protein (BMP-7), or were left unfilled (controls). Three animals per time
period were killed on days 2, 5, 10, 21 and 60 after surgery for each wound type. Cellular proliferation and clonal growth
in periodontal tissues were assessed by 3H-thymidine labeling 1 h before death, followed by radioautography. Cellular differentiation of soft and mineralizing connective
tissue cell populations was determined by immunohistochemical staining of α-smooth muscle actin, osteopontin and bone sialoprotein.
In regenerating periodontium, BMP-7 induced abundant bone formation by 21 days (2.5-fold greater than controls or collagen
implant only; P<0.001), but by day 60 the volume of the newly formed bone had returned to baseline levels and was similar for all groups.
Independent of the type of treatment, periodontal ligament width was unchanged throughout the experimental period (P>0.05). Animals treated with BMP-7 implants showed greatly increased cellular proliferation in the periodontal ligament adjacent
to the wound site and in the regenerating alveolar bone at days 5 and 10 after wounding compared to the other treatment groups
(P<0.005). Animals in the BMP-7 group exhibited similar spatial and temporal staining patterns for α-smooth muscle actin, osteopontin
and bone sialoprotein as controls. Collectively, these data show that BMP-7 promoted the proliferation of precursor cells
in the periodontal ligament but did not induce osteogenic differentiation in this compartment. Consequently a powerful osteogenic
stimulus like BMP-7 cannot significantly perturb the mechanisms that regulate periodontal ligament width and maintain periodontal
homeostasis.
Received: 2 March 1998 / Accepted: 16 June 1998 |
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| Keywords: | Periodontal ligament α -Smooth muscle actin Osteopontin Bone sialoprotein Bone morphogenic protein Rat (Wistar) |
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