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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Research Article Autoimmunity

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 4

Overexpression of soluble human biglycan (7 days) in the liver from transiently transgenic Bgn+/+MRL and Bgn+/+MRL/lpr mice resulted in the presence of human biglycan in plasma and kidneys and caused enhanced albuminuria.

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Overexpression of soluble human biglycan (7 days) in the liver from tran...
(A) Representative RT-PCR from total RNA extracted from the liver of Bgn+/+MRL and Bgn+/+MRL/lpr mice transiently transfected with the pLIVE expression vector plasmid (pLIVE) and pLIVE vector with the inserted human biglycan sequence (hBGN pLIVE). Due to a single SacI restriction site present in the human biglycan gene sequence, digestion of amplified cDNA with SacI resulted in 2 fragments (272 bp and 165 bp) of human (hBGN) compared with a single fragment (428 bp) of murine (mBgn) origin. Mouse Hprt1 was used as a housekeeping gene. (B and C) Western blots for biglycan protein core after semipurification of proteoglycans from plasma (B) and kidney (C) from Bgn+/+MRL and Bgn+/+MRL/lpr mice transiently transfected with hBGN, empty-vector–injected (pLIVE), and control solvent–injected (Cont) mice. Biglycan recovery following purification from plasma and kidneys was linear and varied by 85% ± 6% for all groups. Standards contained 0.3 μg (B) or 0.1 μg (C) of biglycan that was digested with chondroitinase ABC. (D) Urinary albumin/creatinine ratios (μg/mg) in 9-week-old Bgn+/+MRL and Bgn+/+MRL/lpr mice prior to and after 7 days of overexpressing human biglycan (mean ± SD). Asterisk indicates statistical significance; n = 6. *P < 0.05.