Monoallelic IRF5 deficiency in B cells prevents murine lupus
Alex Pellerin, Kei Yasuda, Abraham Cohen-Bucay, Vanessa Sandra, Prachi Shukla, Barry K. Horne Jr, Kerstin Nündel, Gregory A. Viglianti, Yao Xie, Ulf Klein, Ying Tan, Ramon G. Bonegio, Ian R. Rifkin
Alex Pellerin, Kei Yasuda, Abraham Cohen-Bucay, Vanessa Sandra, Prachi Shukla, Barry K. Horne Jr, Kerstin Nündel, Gregory A. Viglianti, Yao Xie, Ulf Klein, Ying Tan, Ramon G. Bonegio, Ian R. Rifkin
View: Text | PDF
Research Article

Monoallelic IRF5 deficiency in B cells prevents murine lupus

Abstract

Gain-of-function polymorphisms in the transcription factor IFN regulatory factor 5 (IRF5) are associated with an increased risk of developing systemic lupus erythematosus. However, the IRF5-expressing cell type(s) responsible for lupus pathogenesis in vivo is not known. We now show that monoallelic IRF5 deficiency in B cells markedly reduced disease in a murine lupus model. In contrast, similar reduction of IRF5 expression in macrophages, monocytes, and neutrophils did not reduce disease severity. B cell receptor and TLR7 signaling synergized to promote IRF5 phosphorylation and increase IRF5 protein expression, with these processes being independently regulated. This synergy increased B cell–intrinsic IL-6 and TNF-α production, both key requirements for germinal center (GC) responses, with IL-6 and TNF-α production in vitro and in vivo being substantially lower with loss of 1 allele of IRF5. Mechanistically, TLR7-dependent IRF5 nuclear translocation was reduced in B cells from IRF5-heterozygous mice. In addition, we show in multiple lupus models that IRF5 expression was dynamically regulated in vivo with increased expression in GC B cells compared with non-GC B cells and with further sequential increases during progression to plasmablasts and long-lived plasma cells. Overall, a critical threshold level of IRF5 in B cells was required to promote disease in murine lupus.

Authors

Alex Pellerin, Kei Yasuda, Abraham Cohen-Bucay, Vanessa Sandra, Prachi Shukla, Barry K. Horne Jr, Kerstin Nündel, Gregory A. Viglianti, Yao Xie, Ulf Klein, Ying Tan, Ramon G. Bonegio, Ian R. Rifkin

×

Figure 4

Decreased renal disease in IRF5ΔB mice.

Options: View larger image (or click on image) Download as PowerPoint
Decreased renal disease in IRF5ΔB mice. All analyses were done in 5-mont...
All analyses were done in 5-month-old FcγRIIB−/−Yaa mice. (A) Representative renal histology of IRF5F/+ and IRF5ΔB mice. Red arrow depicts necrotic cells; black arrow depicts cellular crescent (original magnification, ×20). (BD) Quantification of renal disease by (B) percentage of glomeruli with crescents or necrosis, (C) glomerular injury score, and (D) interstitial disease. IRF5F/+ (n = 11) and IRF5B (n = 8). (E) Representative examples and (F) quantitation of glomerular IgG and complement C3 deposition measured by fluorescence intensity in 11–14 glomeruli per mouse from 5 mice per group. All scored glomeruli are shown (original magnification, ×20). Data are shown as mean ± SEM and were analyzed using 2-tailed, unpaired Welch’s t test; ***P < 0.001, ****P < 0.0001. IRF5, IFN regulatory factor 5.