Inflammatory arthritis increases mouse osteoclast precursors with myeloid suppressor function
Julia F. Charles, Lih-Yun Hsu, Erene C. Niemi, Arthur Weiss, Antonios O. Aliprantis, Mary C. Nakamura
Julia F. Charles, Lih-Yun Hsu, Erene C. Niemi, Arthur Weiss, Antonios O. Aliprantis, Mary C. Nakamura
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Research Article Autoimmunity

Inflammatory arthritis increases mouse osteoclast precursors with myeloid suppressor function

Abstract

Increased osteoclastic bone resorption leads to periarticular erosions and systemic osteoporosis in RA patients. Although a great deal is known about how osteoclasts differentiate from precursors and resorb bone, the identity of an osteoclast precursor (OCP) population in vivo and its regulatory role in RA remains elusive. Here, we report the identification of a CD11b–/loLy6Chi BM population with OCP activity in vitro and in vivo. These cells, which can be distinguished from previously characterized precursors in the myeloid lineage, display features of both M1 and M2 monocytes and expand in inflammatory arthritis models. Surprisingly, in one mouse model of RA (adoptive transfer of SKG arthritis), cotransfer of OCP with SKG CD4+ T cells diminished inflammatory arthritis. Similar to monocytic myeloid-derived suppressor cells (M-MDSCs), OCPs suppressed CD4+ and CD8+ T cell proliferation in vitro through the production of NO. This study identifies a BM myeloid precursor population with osteoclastic and T cell–suppressive activity that is expanded in inflammatory arthritis. Therapeutic strategies that prevent the development of OCPs into mature bone-resorbing cells could simultaneously prevent bone resorption and generate an antiinflammatory milieu in the RA joint.

Authors

Julia F. Charles, Lih-Yun Hsu, Erene C. Niemi, Arthur Weiss, Antonios O. Aliprantis, Mary C. Nakamura

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Figure 6

Adoptive transfer of CD11b-/loLy6Chi OCP does not increase erosive disease, but unexpectedly ameliorates inflammatory arthritis in the adoptive transfer SKG model.

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Adoptive transfer of CD11b-/loLy6Chi OCP does not increase erosive disea...
(A) Schematic of adoptive transfer experiment. Adoptive transfer of conventional SKG CD4+CD25 T cells into Rag2–/– mice typically results in arthritis at 4 weeks. (B) One month after transfer, cross-sectional images from μCT of arthritic ankles were scored blindly for erosions. Coadoptive transfer of OCPs does not increase erosion score compared with mice receiving SKG CD4+ cells alone. Few erosions are seen in the group receiving Tregs. (C) Representative cross-sectional images used for erosion scoring; star denotes an erosion. (D) Blinded arthritis scores are significantly ameliorated by coadoptive transfer of CD11b–/loLy6Chi OCP compared with CD4+ group, although not as dramatically as with cotransfer of wild-type Tregs. *P = 0.03, Student’s t test. (E) Representative images from sagittal ankle sections shows inflammatory changes in the marrow of both OCP and CD4+ groups (stars), but more prominent synovial infiltrate (arrowheads) in the CD4+ group. H&E staining. Original magnification, ×10.