Signaling pathways predisposing to chronic kidney disease progression
Mohamad Zaidan, … , Marco Pontoglio, Fabiola Terzi
Mohamad Zaidan, … , Marco Pontoglio, Fabiola Terzi
Published May 7, 2020
Citation Information: JCI Insight. 2020;5(9):e126183. https://doi.org/10.1172/jci.insight.126183.
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Research Article Nephrology

Signaling pathways predisposing to chronic kidney disease progression

Abstract

The loss of functional nephrons after kidney injury triggers the compensatory growth of the remaining ones to allow functional adaptation. However, in some cases, these compensatory events activate signaling pathways that lead to pathological alterations and chronic kidney disease. Little is known about the identity of these pathways and how they lead to the development of renal lesions. Here, we combined mouse strains that differently react to nephron reduction with molecular and temporal genome-wide transcriptome studies to elucidate the molecular mechanisms involved in these events. We demonstrated that nephron reduction led to 2 waves of cell proliferation: the first one occurred during the compensatory growth regardless of the genetic background, whereas the second one occurred, after a quiescent phase, exclusively in the sensitive strain and accompanied the development of renal lesions. Similarly, clustering by coinertia analysis revealed the existence of 2 waves of gene expression. Interestingly, we identified type I interferon (IFN) response as an early (first-wave) and specific signature of the sensitive (FVB/N) mice. Activation of type I IFN response was associated with G1/S cell cycle arrest, which correlated with p21 nuclear translocation. Remarkably, the transient induction of type I IFN response by poly(I:C) injections during the compensatory growth resulted in renal lesions in otherwise-resistant C57BL6 mice. Collectively, these results suggest that the early molecular and cellular events occurring after nephron reduction determine the risk of developing late renal lesions and point to type I IFN response as a crucial event of the deterioration process.

Authors

Mohamad Zaidan, Martine Burtin, Jitao David Zhang, Thomas Blanc, Pauline Barre, Serge Garbay, Clément Nguyen, Florence Vasseur, Lucie Yammine, Serena Germano, Laura Badi, Marie-Claire Gubler, Morgan Gallazzini, Gérard Friedlander, Marco Pontoglio, Fabiola Terzi

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Figure 2

Temporal unbiased transcriptomic analysis revealed a distinct pattern of gene expression in sensitive and resistant strains.

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Temporal unbiased transcriptomic analysis revealed a distinct pattern of...
(A) Animal clustering using coinertia analysis. Sample partition by the 2 principal components (PCs): strain (dotted line, PC1) and surgery (dotted/dashed line, PC2); n = 4 mice per group (S, sham operation; N, subtotal nephrectomy) from each strain (C, B6; F, FVB) at each time point (2, 28, and 56 days). (B) Scatter plots comparing the amplitude of differential gene expression between FVB (y axis) and B6 mice (x axis) 2, 28, and 56 days after sham operation (Sh) or subtotal nephrectomy (Nx). Each point represents a single gene. The correlation coefficient (cor) is indicated in each panel.