Protein kinase N3 promotes bone resorption by osteoclasts in response to Wnt5a-Ror2 signaling.
Shunsuke UeharaNobuyuki UdagawaHideyuki MukaiAkihiro IshiharaKazuhiro MaedaTeruhito YamashitaKohei MurakamiMichiru NishitaTakashi NakamuraShigeaki KatoYasuhiro MinamiNaoyuki TakahashiYasuhiro KobayashiPublished in: Science signaling (2017)
Cytoskeletal reorganization in osteoclasts to form actin rings is necessary for these cells to attach to bone and resorb bone matrices. We delineated the pathway through which Wnt5a signaling through receptor tyrosine kinase-like orphan receptor 2 (Ror2) promoted the bone-resorbing activity of osteoclasts. Wnt5a binding to Ror2 stimulated Rho, a small GTPase involved in cytoskeletal reorganization. Subsequently, the Rho effector kinase Pkn3 bound to and enhanced the activity of c-Src, a nonreceptor tyrosine kinase that is critical for actin ring formation. Mice with an osteoclast-specific deficiency in Ror2 (Ror2ΔOcl/ΔOcl) had increased bone mass. Osteoclasts derived from these mice exhibited impaired bone resorption and actin ring formation, defects that were rescued by overexpression of constitutively active RhoA. These osteoclasts also exhibited reduced interaction between c-Src and Pkn3 and reduced c-Src kinase activity. Similar to Ror2ΔOcl/ΔOcl mice, mice with a global deficiency of Pkn3 (Pkn3-/-) had increased bone mass. The proline-rich region and kinase domain of Pkn3 were required to restore the bone-resorbing activity of osteoclasts derived from Pkn3-/- mice. Thus, Pkn3 promotes bone resorption downstream of Wnt5a-Ror2-Rho signaling, and this pathway may be a therapeutic target for bone diseases such as osteoporosis, rheumatoid arthritis, and periodontal disease.
Keyphrases
- bone loss
- tyrosine kinase
- bone mineral density
- protein kinase
- soft tissue
- epidermal growth factor receptor
- rheumatoid arthritis
- cell proliferation
- high fat diet induced
- stem cells
- body composition
- skeletal muscle
- type diabetes
- adipose tissue
- idiopathic pulmonary fibrosis
- cell death
- transcription factor
- immune response
- systemic sclerosis
- signaling pathway
- regulatory t cells