| Literature DB >> 24899055 |
Yoshikuni Nagayama1, Gerald S Braun2, Christina M Jakobs3, Yuichi Maruta1, Claudia R van Roeyen3, Barbara M Klinkhammer3, Peter Boor4, Luigi Villa3, Ute Raffetseder3, Christian Trautwein5, Dieter Görtz6, Gerhard Müller-Newen6, Tammo Ostendorf3, Jürgen Floege3.
Abstract
Renal inflammation, in particular glomerular, is often characterized by increased IL-6 levels. The in vivo relevance of IL-6 signaling in glomerular podocytes, which play central roles in most glomerular diseases, is unknown. Here, we show that in normal mice, podocytes express gp130, the common signal-transducing receptor subunit of the IL-6 family of cytokines. Following systemic IL-6 or LPS injection in mice, podocyte IL-6 signaling was evidenced by downstream STAT3 phosphorylation. Next, we generated mice deficient for gp130 in podocytes. Expectedly, these mice exhibited abrogated IL-6 downstream signaling in podocytes. At the age of 40 wk, they did not show spontaneous renal pathology or abnormal renal function. The mice were then challenged using two LPS injury models as well as nephrotoxic serum to induce crescentic nephritis. Under all conditions, circulating IL-6 levels increased markedly and the mice developed the pathological hallmarks of the corresponding injury models such as proteinuria and development of glomerular crescents, respectively. However, despite the capacity of normal podocytes to transduce IL-6 family signals downstream, there were no significant differences between mice bearing the podocyte-specific gp130 deletion and their control littermates in any of these models. In conclusion, under the different conditions tested, gp130 signaling was not a critical component of the (patho-)biology of the podocyte in vivo.Entities:
Keywords: crescentic nephritis; glomerulus; gp130; lipopolysaccharide; pSTAT3
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Year: 2014 PMID: 24899055 DOI: 10.1152/ajprenal.00620.2013
Source DB: PubMed Journal: Am J Physiol Renal Physiol ISSN: 1522-1466