Naslov
An EP2 receptor-selective prostaglandin E2 agonist induces bone healing

Autori
Paralkar, V.M. ; Borovečki, Fran ; Ke, H.Z. ; Cameron, K.O. ; Lefker, B. ; Grasser W.A. ; Owen, T.A. ; Li, M. ; DaSilva-Jardine, P. ; Zhou, M. ; Dunn, R.L. ; Dumont, F. ; Korsmeyer, R. ; Krasney, P. ; Brown, T.A. ; Plowchalk, D. ; Vukičević, Slobodan ; Thompson, D.D.

Izvornik
Proceedings of the National Academy of Sciences of the United States of America (0027-8424) 100 (2003), 11; 6736-40.

Vrsta, podvrsta i kategorija rada
Radovi u časopisima, članak, znanstveni

Ključne riječi
PGE2; EP2 receptor selective agonist; long bone segmental defect

Sažetak
The morbidity and mortality associated with impaired/delayed fracture healing remain high. Our objective was to identify a small nonpeptidyl molecule with the ability to promote fracture healing and prevent malunions. Prostaglandin E2 (PGE2) causes significant increases in bone mass and bone strength when administered systemically or locally to the skeleton. However, due to side effects, PGE2 is an unacceptable therapeutic option for fracture healing. PGE2 mediates its tissue-specific pharmacological activity via four different G protein-coupled receptor subtypes, EP1, -2, -3, and -4. The anabolic action of PGE2 in bone has been linked to an elevated level of cAMP, thereby implicating the EP2 and/or EP4 receptor subtypes in bone formation. We identified an EP2 selective agonist, CP-533, 536, which has the ability to heal canine long bone segmental and fracture model defects without the objectionable side effects of PGE2, suggesting that the EP2 receptor subtype is a major contributor to PGE2's local bone anabolic activity. The potent bone anabolic activity of CP-533, 536 offers a therapeutic alternative for the treatment of fractures and bone defects in patients.

Izvorni jezik
Engleski

Znanstvena područja
Temeljne medicinske znanosti

POVEZANOST RADA