| Literature DB >> 17316789 |
Takatoshi Okuda1, Koji Ioku, Ikuho Yonezawa, Hideyuki Minagi, Giichiro Kawachi, Yoshinori Gonda, Hisashi Murayama, Yasuaki Shibata, Soichiro Minami, Shimeru Kamihira, Hisashi Kurosawa, Tohru Ikeda.
Abstract
The response of bone cells to a newly developed porous beta-tricalcium phosphate composed of rod-shaped particles (RSbeta-TCP), beta-TCP composed of conventional non-rod-shaped particles (Cbeta-TCP), and hydroxyapatite (HA) was analyzed using in vivo implantation and in vitro osteoclastogenesis systems. Implantation of the materials into the rabbit femur showed that RSbeta-TCP and Cbeta-TCP were bioresorbable, but HA was not. Up to 12 weeks after the implantation, bioresorption of RSbeta-TCP and Cbeta-TCP accompanied by the formation of new bone occurred satisfactorily. At 24 weeks post-implantation, most of the RSbeta-TCP had been absorbed, and active osteogenesis was preserved in the region. However, in the specimens implanted with Cbeta-TCP, the amount of not only the implanted Cbeta-TCP but also the newly formed bone tissue decreased, and bone marrow dominated the region. The implanted HA was unbioresorbable throughout the experimental period. When osteoclasts were generated on RSbeta-TCP, Cbeta-TCP, or HA disks, apparent resorption lacunae were formed on the RSbeta-TCP and Cbeta-TCP, but not HA disks. Quantitation of the calcium concentration in the culture media showed an earlier and more constant release of calcium from RSbeta-TCP than Cbeta-TCP. These results showed that the microstructure of beta-TCP affects the activity of bone cells and subsequent bone replacement.Entities:
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Year: 2007 PMID: 17316789 DOI: 10.1016/j.biomaterials.2007.01.040
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479