Cell Reports (Oct 2014)

Nonclassical Ly6C− Monocytes Drive the Development of Inflammatory Arthritis in Mice

  • Alexander V. Misharin,
  • Carla M. Cuda,
  • Rana Saber,
  • Jason D. Turner,
  • Angelica K. Gierut,
  • G. Kenneth Haines III,
  • Sergejs Berdnikovs,
  • Andrew Filer,
  • Andrew R. Clark,
  • Christopher D. Buckley,
  • Gökhan M. Mutlu,
  • G.R. Scott Budinger,
  • Harris Perlman

DOI
https://doi.org/10.1016/j.celrep.2014.09.032
Journal volume & issue
Vol. 9, no. 2
pp. 591 – 604

Abstract

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Different subsets and/or polarized phenotypes of monocytes and macrophages may play distinct roles during the development and resolution of inflammation. Here, we demonstrate in a murine model of rheumatoid arthritis that nonclassical Ly6C− monocytes are required for the initiation and progression of sterile joint inflammation. Moreover, nonclassical Ly6C− monocytes differentiate into inflammatory macrophages (M1), which drive disease pathogenesis and display plasticity during the resolution phase. During the development of arthritis, these cells polarize toward an alternatively activated phenotype (M2), promoting the resolution of joint inflammation. The influx of Ly6C− monocytes and their subsequent classical and then alternative activation occurs without changes in synovial tissue-resident macrophages, which express markers of M2 polarization throughout the course of the arthritis and attenuate joint inflammation during the initiation phase. These data suggest that circulating Ly6C− monocytes recruited to the joint upon injury orchestrate the development and resolution of autoimmune joint inflammation.