MIP-1γ Promotes Receptor Activator of NF-κB Ligand-Induced Osteoclast Formation and Survival

  • Yoshimasa Okamatsu
    *Department of Cytokine Biology, Forsyth Institute, Boston, MA 02115; and
  • David Kim
    *Department of Cytokine Biology, Forsyth Institute, Boston, MA 02115; and
  • Ricardo Battaglino
    *Department of Cytokine Biology, Forsyth Institute, Boston, MA 02115; and
  • Hajime Sasaki
    *Department of Cytokine Biology, Forsyth Institute, Boston, MA 02115; and
  • Ulrike Späte
    *Department of Cytokine Biology, Forsyth Institute, Boston, MA 02115; and
  • Philip Stashenko
    *Department of Cytokine Biology, Forsyth Institute, Boston, MA 02115; and

説明

<jats:title>Abstract</jats:title> <jats:p>Chemokines play an important role in immune and inflammatory responses by inducing migration and adhesion of leukocytes, and have also been reported to modulate osteoclast differentiation from hemopoietic precursor cells of the monocyte-macrophage lineage. In this study, we examined the effect of MIP-1γ, a C-C chemokine family member, on receptor activator of NF-κB ligand (RANKL)-stimulated osteoclast differentiation, survival, and activation. RANKL induced osteoclasts to dramatically increase production of MIP-1γ and to also express the MIP-1γ receptor CCR1, but had only minor effects on the related C-C chemokines MIP-1α and RANTES. Neutralization of MIP-1γ with specific Ab reduced RANKL-stimulated osteoclast differentiation by 60–70%. Mature osteoclasts underwent apoptosis within 24 h after removal of RANKL, as shown by increased caspase 3 activity and DNA fragmentation. Apoptosis was reduced by the addition of exogenous MIP-1γ or RANKL, both of which increased NF-κB activation in osteoclasts. Neutralization studies showed that the prosurvival effect of RANKL was in part dependent on its ability to induce MIP-1γ. Finally, osteoclast activation for bone resorption was stimulated by MIP-1γ. Taken together, these results demonstrate that MIP-1γ plays an important role in the differentiation and survival of osteoclasts, most likely via an autocrine pathway.</jats:p>

収録刊行物

  • The Journal of Immunology

    The Journal of Immunology 173 (3), 2084-2090, 2004-08-01

    The American Association of Immunologists

被引用文献 (6)*注記

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