B cell–intrinsic TLR9 expression is protective in murine lupus
Jeremy S. Tilstra, … , Kevin M. Nickerson, Mark J. Shlomchik
Jeremy S. Tilstra, … , Kevin M. Nickerson, Mark J. Shlomchik
Published March 19, 2020
Citation Information: J Clin Invest. 2020;130(6):3172-3187. https://doi.org/10.1172/JCI132328.
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B cell–intrinsic TLR9 expression is protective in murine lupus

Abstract

Toll-like receptor 9 (TLR9) is a regulator of disease pathogenesis in systemic lupus erythematosus (SLE). Why TLR9 represses disease while TLR7 and MyD88 have the opposite effect remains undefined. To begin to address this question, we created 2 alleles to manipulate TLR9 expression, allowing for either selective deletion or overexpression. We used these to test cell type–specific effects of Tlr9 expression on the regulation of SLE pathogenesis. Notably, Tlr9 deficiency in B cells was sufficient to exacerbate nephritis while extinguishing anti–nucleosome antibodies, whereas Tlr9 deficiency in dendritic cells (DCs), plasmacytoid DCs, and neutrophils had no discernable effect on disease. Thus, B cell–specific Tlr9 deficiency unlinked disease from autoantibody production. Critically, B cell–specific Tlr9 overexpression resulted in ameliorated nephritis, opposite of the effect of deleting Tlr9. Our findings highlight the nonredundant role of B cell–expressed TLR9 in regulating lupus and suggest therapeutic potential in modulating and perhaps even enhancing TLR9 signals in B cells.

Authors

Jeremy S. Tilstra, Shinu John, Rachael A. Gordon, Claire Leibler, Michael Kashgarian, Sheldon Bastacky, Kevin M. Nickerson, Mark J. Shlomchik

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Figure 2

B cell–specific TLR9 deficiency results in exacerbated renal disease.

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B cell–specific TLR9 deficiency results in exacerbated renal disease. (A...
(A) Schematic representation of Tlr9 floxed allele generation. Exons (open rectangles), LoxP sites (black triangles), FLP recombinase target sites (block open arrowheads) are also shown. (B) Sorted B cells from control or CD19-Cre Tlr9fl/fl mice were stimulated with CpG ODN 1826 (5 μg/mL) for 3 days and IgM secretion was quantified by ELISA (n = 2 per group). Scatter plots display data from individual mice with black lines showing means. **P < 0.01 using the 2-tailed Student’s t test. Phenotypic markers were assessed in 16-week-old MRL/lpr mice from each indicated genotype, including (C) proteinuria, (D) glomerular renal disease, (E) interstitial and perivascular renal infiltrates, with (F) representative images of H&E kidney sections from mice of indicated genotype, where black arrowheads indicate interstitial inflammation and white arrows show glomeruli. Additional phenotypic endpoints were assessed for each noted genotype including (G) dermatitis, (H) spleen weight, and (I) lymph node weight. Controls: n = 24–31; CD19-Cre Tlr9fl/fl: n = 19–24. Scatter plots display data from individual mice with black lines showing median values. *P < 0.05, 2-tailed Mann-Whitney U test.