Locally delivered rhBMP‐2 enhances bone ingrowth and gap healing in a canine model

The purpose of the present study was to determine if recombinant human bone morphogenetic protein‐2 (rhBMP‐2) enhances bone ingrowth into porous‐coated implants and gap healing around the implants. In the presence of a 3‐mm gap between the implant and host bone, porous‐coated implants were placed bilaterally for four weeks in the proximal humeri of skeletally mature, adult male dogs. In three treatment groups, the test implant was treated with HA/TCP and rhBMP‐2 in buffer at a dose of 100 μg/implant ( n = 5), 400 μg/implant ( n = 6), or 800 μg/implant ( n = 5) and placed in the left humerus. In these same animals, an internal control implant was treated only with HA/TCP and buffer and placed in the right humerus. These groups were compared with a previously reported external control group of seven animals in which no growth factor was delivered [J. Orthop. Res. 19 (2001) 85]. The BMP treated implants in the two lower dose groups had significantly more bone ingrowth than the external controls with the greatest effect in the 100 g/implant group (a 3.5‐fold increase over the external control, p = 0.008). All three dose groups had significantly more bone formation in the 3‐mm gap surrounding the BMP treated implants than the external controls with the greatest effect in the 800 μg group (2.9‐fold increase, p < 0.001). Thus, application of rhBMP‐2 to a porous‐coated implant stimulated local bone ingrowth and gap healing. The enhancement of bone formation within the implant (bone ingrowth) was inversely related to dose. © 2003 Orthopaedic Research Society. Published by Elsevier Ltd. All rights reserved.