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PGC-1α promotes recovery after acute kidney injury during systemic inflammation in mice
Mei Tran, … , Zoltan Arany, Samir M. Parikh
Mei Tran, … , Zoltan Arany, Samir M. Parikh
Published September 1, 2011
Citation Information: J Clin Invest. 2011;121(10):4003-4014. https://doi.org/10.1172/JCI58662.
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Research Article Nephrology

PGC-1α promotes recovery after acute kidney injury during systemic inflammation in mice

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Abstract

Sepsis-associated acute kidney injury (AKI) is a common and morbid condition that is distinguishable from typical ischemic renal injury by its paucity of tubular cell death. The mechanisms underlying renal dysfunction in individuals with sepsis-associated AKI are therefore less clear. Here we have shown that endotoxemia reduces oxygen delivery to the kidney, without changing tissue oxygen levels, suggesting reduced oxygen consumption by the kidney cells. Tubular mitochondria were swollen, and their function was impaired. Expression profiling showed that oxidative phosphorylation genes were selectively suppressed during sepsis-associated AKI and reactivated when global function was normalized. PPARγ coactivator–1α (PGC-1α), a major regulator of mitochondrial biogenesis and metabolism, not only followed this pattern but was proportionally suppressed with the degree of renal impairment. Furthermore, tubular cells had reduced PGC-1α expression and oxygen consumption in response to TNF-α; however, excess PGC-1α reversed the latter effect. Both global and tubule-specific PGC-1α–knockout mice had normal basal renal function but suffered persistent injury following endotoxemia. Our results demonstrate what we believe to be a novel mechanism for sepsis-associated AKI and suggest that PGC-1α induction may be necessary for recovery from this disorder, identifying a potential new target for future therapeutic studies.

Authors

Mei Tran, Denise Tam, Amit Bardia, Manoj Bhasin, Glenn C. Rowe, Ajay Kher, Zsuzsanna K. Zsengeller, M. Reza Akhavan-Sharif, Eliyahu V. Khankin, Magali Saintgeniez, Sascha David, Deborah Burstein, S. Ananth Karumanchi, Isaac E. Stillman, Zoltan Arany, Samir M. Parikh

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Figure 3

Similarities in expression profiles between early and persistent injury and between baseline and recovery states.

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Similarities in expression profiles between early and persistent injury ...
(A) Eighteen hours after LPS, mice received 10 ml/kg saline, and by 42 hours after LPS, the majority had recovered from AKI. Kidneys from n = 3 animals per indicated condition (baseline, early injury, persistent injury, recovery; red circles) were studied by expression profiling. Dashed horizontal lines indicate mean values. (B) PCA of the transcriptional data from each condition. The percentage values indicate the proportion of total variance described by the corresponding principal component. (C) Genes were selected using supervised analysis on the basis of 1-way ANOVA of the 4 conditions — baseline, early injury, persistent injury, and recovery. Columns represent the samples, and rows represent the genes, with expression demonstrated by pseudocolor scale (–3 = green, +3 = red).

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