JCI Insight (Nov 2020)

Pathogenic, glycolytic PD-1+ B cells accumulate in the hypoxic RA joint

  • Achilleas Floudas,
  • Nuno Neto,
  • Viviana Marzaioli,
  • Kieran Murray,
  • Barry Moran,
  • Michael G. Monaghan,
  • Candice Low,
  • Ronan H. Mullan,
  • Navin Rao,
  • Vinod Krishna,
  • Sunil Nagpal,
  • Douglas J. Veale,
  • Ursula Fearon

Journal volume & issue
Vol. 5, no. 21

Abstract

Read online

While autoantibodies are used in the diagnosis of rheumatoid arthritis (RA), the function of B cells in the inflamed joint remains elusive. Extensive flow cytometric characterization and SPICE algorithm analyses of single-cell synovial tissue from patients with RA revealed the accumulation of switched and double-negative memory programmed death-1 receptor–expressing (PD-1–expressing) B cells at the site of inflammation. Accumulation of memory B cells was mediated by CXCR3, evident by the observed increase in CXCR3-expressing synovial B cells compared with the periphery, differential regulation by key synovial cytokines, and restricted B cell invasion demonstrated in response to CXCR3 blockade. Notably, under 3% O2 hypoxic conditions that mimic the joint microenvironment, RA B cells maintained marked expression of MMP-9, TNF, and IL-6, with PD-1+ B cells demonstrating higher expression of CXCR3, CD80, CD86, IL-1β, and GM-CSF than their PD-1– counterparts. Finally, following functional analysis and flow cell sorting of RA PD-1+ versus PD-1– B cells, we demonstrate, using RNA-Seq and emerging fluorescence lifetime imaging microscopy of cellular NAD, a significant shift in metabolism of RA PD-1+ B cells toward glycolysis, associated with an increased transcriptional signature of key cytokines and chemokines that are strongly implicated in RA pathogenesis. Our data support the targeting of pathogenic PD-1+ B cells in RA as a focused, novel therapeutic option.

Keywords