Scientific Reports (Feb 2018)

CD38 promotes pristane-induced chronic inflammation and increases susceptibility to experimental lupus by an apoptosis-driven and TRPM2-dependent mechanism

  • Sonia García-Rodríguez,
  • Antonio Rosal-Vela,
  • Davide Botta,
  • Luz M. Cumba Garcia,
  • Esther Zumaquero,
  • Verónica Prados-Maniviesa,
  • Daniela Cerezo-Wallis,
  • Nicola Lo Buono,
  • José-Ángel Robles-Guirado,
  • Salvador Guerrero,
  • Elena González-Paredes,
  • Eduardo Andrés-León,
  • Ángel Corbí,
  • Matthias Mack,
  • Friedrich Koch-Nolte,
  • Ramón Merino,
  • Mercedes Zubiaur,
  • Frances E. Lund,
  • Jaime Sancho

DOI
https://doi.org/10.1038/s41598-018-21337-6
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 19

Abstract

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Abstract In this study, we investigated the role of CD38 in a pristane-induced murine model of lupus. CD38-deficient (Cd38 −/−) but not ART2-deficient (Art2 −/−) mice developed less severe lupus compared to wild type (WT) mice, and their protective phenotype consisted of (i) decreased IFN-I-stimulated gene expression, (ii) decreased numbers of peritoneal CCR2hiLy6Chi inflammatory monocytes, TNF-α-producing Ly6G+ neutrophils and Ly6Clo monocytes/macrophages, (iii) decreased production of anti-single-stranded DNA and anti-nRNP autoantibodies, and (iv) ameliorated glomerulonephritis. Cd38 −/− pristane-elicited peritoneal exudate cells had defective CCL2 and TNF-α secretion following TLR7 stimulation. However, Tnf-α and Cxcl12 gene expression in Cd38 −/− bone marrow (BM) cells was intact, suggesting a CD38-independent TLR7/TNF-α/CXCL12 axis in the BM. Chemotactic responses of Cd38 −/− Ly6Chi monocytes and Ly6G+ neutrophils were not impaired. However, Cd38 −/− Ly6Chi monocytes and Ly6Clo monocytes/macrophages had defective apoptosis-mediated cell death. Importantly, mice lacking the cation channel TRPM2 (Trpm2 −/−) exhibited very similar protection, with decreased numbers of PECs, and apoptotic Ly6Chi monocytes and Ly6Clo monocytes/macrophages compared to WT mice. These findings reveal a new role for CD38 in promoting aberrant inflammation and lupus-like autoimmunity via an apoptosis-driven mechanism. Furthermore, given the implications of CD38 in the activation of TRPM2, our data suggest that CD38 modulation of pristane-induced apoptosis is TRPM2-dependent.