Lipocalin-2 derived from adipose tissue mediates aldosterone-induced renal injury
Wai Yan Sun, Bo Bai, Cuiting Luo, Kangmin Yang, Dahui Li, Donghai Wu, Michel Félétou, Nicole Villeneuve, Yang Zhou, Junwei Yang, Aimin Xu, Paul M. Vanhoutte, Yu Wang
Wai Yan Sun, Bo Bai, Cuiting Luo, Kangmin Yang, Dahui Li, Donghai Wu, Michel Félétou, Nicole Villeneuve, Yang Zhou, Junwei Yang, Aimin Xu, Paul M. Vanhoutte, Yu Wang
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Research Article Inflammation Nephrology

Lipocalin-2 derived from adipose tissue mediates aldosterone-induced renal injury

Abstract

Lipocalin-2 is not only a sensitive biomarker, but it also contributes to the pathogenesis of renal injuries. The present study demonstrates that adipose tissue–derived lipocalin-2 plays a critical role in causing both chronic and acute renal injuries. Four-week treatment with aldosterone and high salt after uninephrectomy (ANS) significantly increased both circulating and urinary lipocalin-2, and it induced glomerular and tubular injuries in kidneys of WT mice. Despite increased renal expression of lcn2 and urinary excretion of lipocalin-2, mice with selective deletion of lcn2 alleles in adipose tissue (Adipo-LKO) are protected from ANS- or aldosterone-induced renal injuries. By contrast, selective deletion of lcn2 alleles in kidney did not prevent aldosterone- or ANS-induced renal injuries. Transplantation of fat pads from WT donors increased the sensitivity of mice with complete deletion of Lcn2 alleles (LKO) to aldosterone-induced renal injuries. Aldosterone promoted the urinary excretion of a human lipocalin-2 variant, R81E, in turn causing renal injuries in LKO mice. Chronic treatment with R81E triggered significant renal injuries in LKO, resembling those observed in WT mice following ANS challenge. Taken in conjunction, the present results demonstrate that lipocalin-2 derived from adipose tissue causes acute and chronic renal injuries, largely independent of local lcn2 expression in kidney.

Authors

Wai Yan Sun, Bo Bai, Cuiting Luo, Kangmin Yang, Dahui Li, Donghai Wu, Michel Félétou, Nicole Villeneuve, Yang Zhou, Junwei Yang, Aimin Xu, Paul M. Vanhoutte, Yu Wang

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Figure 3

Deficiency of lipocalin-2 protects mice from ANS-induced tubular injuries in the kidney.

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Deficiency of lipocalin-2 protects mice from ANS-induced tubular injurie...
(A) WT, Adipo-LKO, and LKO mice were subjected to sham or ANS treatment as in Figure 1. Morphological changes of renal tubules were examined by H&E (upper row) or PAS (lower row) staining. Images of proximal tubules in the cortex are shown. Magnification, 400×. Scale bar: 20 μm. (B) Quantification of tubular cell height and diameter was performed using ImageJ software. (C) Ten random images from 1 animal were examined to calculate the average data for comparison. The mRNA expression levels of clu and kim-1 in kidney samples were measured by qPCR and presented as fold changes against WT sham controls. (D) The protein amount of Kim-1 in the 24-hour urine samples was measured by ELISA for comparison. Data are shown as mean ± SEM; *P < 0.05 vs. WT sham controls; #P < 0.05 vs. WT ANS by Mann-Whitney nonparametric Student’s t test(n = 6–8). EPL, Eplerenone.