TLR4 activation mediates kidney ischemia/reperfusion injury
Huiling Wu, … , Alexandra F. Sharland, Steven J. Chadban
Huiling Wu, … , Alexandra F. Sharland, Steven J. Chadban
Published October 1, 2007
Citation Information: J Clin Invest. 2007;117(10):2847-2859. https://doi.org/10.1172/JCI31008.
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TLR4 activation mediates kidney ischemia/reperfusion injury

Abstract

Ischemia/reperfusion injury (IRI) may activate innate immunity through the engagement of TLRs by endogenous ligands. TLR4 expressed within the kidney is a potential mediator of innate activation and inflammation. Using a mouse model of kidney IRI, we demonstrated a significant increase in TLR4 expression by tubular epithelial cells (TECs) and infiltrating leukocytes within the kidney following ischemia. TLR4 signaling through the MyD88-dependent pathway was required for the full development of kidney IRI, as both TLR4–/– and MyD88–/– mice were protected against kidney dysfunction, tubular damage, neutrophil and macrophage accumulation, and expression of proinflammatory cytokines and chemokines. In vitro, WT kidney TECs produced proinflammatory cytokines and chemokines and underwent apoptosis after ischemia. These effects were attenuated in TLR4–/– and MyD88–/– TECs. In addition, we demonstrated upregulation of the endogenous ligands high-mobility group box 1 (HMGB1), hyaluronan, and biglycan, providing circumstantial evidence that one or more of these ligands may be the source of TLR4 activation. To determine the relative contribution of TLR4 expression by parenchymal cells or leukocytes to kidney damage during IRI, we generated chimeric mice. TLR4–/– mice engrafted with WT hematopoietic cells had significantly lower serum creatinine and less tubular damage than WT mice reconstituted with TLR4–/– BM, suggesting that TLR4 signaling in intrinsic kidney cells plays the dominant role in mediating kidney damage.

Authors

Huiling Wu, Gang Chen, Kate R. Wyburn, Jianlin Yin, Patrick Bertolino, Josette M. Eris, Stephen I. Alexander, Alexandra F. Sharland, Steven J. Chadban

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Figure 2

TLR protein expression is increased in the kidney following ischemia/reperfusion.

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TLR protein expression is increased in the kidney following ischemia/rep...
(A) Immunostaining demonstrated that TLR4 protein was expressed by infiltrating cells and TECs at day 1 and then predominantly expressed by TECs on days 3, 5, and 9 after IRI. Original magnification, ×200. (B) TLR4 was expressed by intrarenal leukocyte cells at day 1 after IRI. Magnification, ×600. (C) TLR4 was expressed by tubular cells at day 5 after IRI. Original magnification, ×600. (D) The number of cells expressing TLR4 dramatically increased on day 1, declining rapidly thereafter. These cells could be resident renal DCs/macrophages or infiltrating leukocytes. (E) Expression levels of TLR4 protein in tubules were significantly increased from day 1 to day 9 after IRI compared with sham-operated controls. **P < 0.01; ***P < 0.001. Data are mean ± SD. n = 6–8 per group.