The proteoglycan biglycan regulates expression of the B cell chemoattractant CXCL13 and aggravates murine lupus nephritis
Kristin Moreth, … , Roland M. Schaefer, Liliana Schaefer
Kristin Moreth, … , Roland M. Schaefer, Liliana Schaefer
Published November 15, 2010
Citation Information: J Clin Invest. 2010;120(12):4251-4272. https://doi.org/10.1172/JCI42213.
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The proteoglycan biglycan regulates expression of the B cell chemoattractant CXCL13 and aggravates murine lupus nephritis

Abstract

CXCL13 is a key B cell chemoattractant and marker of disease activity in patients with SLE; however, the mechanism of its induction has not been identified yet. Here, we have shown that the proteoglycan biglycan triggers CXCL13 expression via TLR2/4 in macrophages and dendritic cells. In vivo, levels of biglycan were markedly elevated in the plasma and kidneys of human SLE patients and lupus-prone (MRL/lpr) mice. Overexpression of soluble biglycan in MRL/lpr mice raised plasma and renal levels of CXCL13 and caused accumulation of B cells with an enhanced B1/B cell ratio in the kidney, worsening of organ damage, and albuminuria. Importantly, biglycan also triggered CXCL13 expression and B cell infiltration in the healthy kidney. Conversely, biglycan deficiency improved systemic and renal outcome in lupus-prone mice, with lower levels of autoantibodies, less enlargement of the spleen and lymph nodes, and reduction in renal damage and albuminuria. This correlated with a marked decline in circulating and renal CXCL13 and a reduction in the number of B cells in the kidney. Collectively, our results describe what we believe to be a novel mechanism for the regulation of CXCL13 by biglycan, a host-derived ligand for TLR2/4. Blocking biglycan-TLR2/4 interactions might be a promising strategy for the management of SLE and other B cell–mediated inflammatory disease entities.

Authors

Kristin Moreth, Rebekka Brodbeck, Andrea Babelova, Norbert Gretz, Tilmann Spieker, Jinyang Zeng-Brouwers, Josef Pfeilschifter, Marian F. Young, Roland M. Schaefer, Liliana Schaefer

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Figure 8

Effects of biglycan expression on the B cell chemoattractant CXCL13 in kidneys, plasma, and resident peritoneal macrophages from MRL/lpr mice.

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Effects of biglycan expression on the B cell chemoattractant CXCL13 in k...
Ten-week-old Bgn+/+MRL, Bgn+/+MRL/lpr, Bgn–/–MRL/lpr, hBGN, mice and their respective controls, as well as 16- and 24-week-old Bgn–/–MRL/lpr and Bgn+/+MRL/lpr mice were analyzed for Cxcl13 expression and content in total kidney homogenates and plasma, as well as for the renal expression of Cxcr5. (A and D) TaqMan analysis for the renal expression of Cxcl13 (A) and its receptor Cxcr5 (D) shown as the average fold induction relative to controls (Bgn+/+MRL) (normalized to Gapdh) and (B and C) ELISA for CXCL13 from total kidney homogenates normalized to total protein (B) and from plasma (C). There were no differences in CXCL13 expression and levels between Bgn+/+MRL and Bgn–/–MRL mice (AD). (E and F) TaqMan analysis (E) and ELISA (F) for CXCL13 in peritoneal macrophages (E) or their culture supernatants (F) from 16-week-old Bgn–/–MRL/lpr and Bgn+/+MRL/lpr mice versus Bgn+/+MRL control mice. To measure the expression (E) and levels of CXCL13 in culture supernatants (F), monocytes/macrophages were flushed from the peritoneal cavity and plated (2 × 105) under serum-free conditions for 12 hours and cells (E) or culture supernatants (F) were analyzed for CXCL13. TaqMan results (E) are given as average fold induction relative to control, normalized to Gapdh. Asterisks indicate statistical significance; n = 6. *P < 0.05. Data are given as mean ± SD.