Disruption of Renal Arginine Metabolism Promotes Kidney Injury in Hepatorenal Syndrome in Mice.

Zoltan V VargaKatalin ErdelyiJanos PalocziResat CinarZsuzsanna K ZsengellerTony JourdanCsaba MatyasBalazs Tamas NemethAdrien GuillotXiaogang XiangAdam MehalGyörgy HaskóIsaac E StillmanSeymour RosenBin GaoGeorge KunosPal Pacher

Published in: Hepatology (Baltimore, Md.) (2019)

We propose that hyperammonemia may contribute to impaired renal arginine metabolism, leading to decreased eNOS activity, impaired microcirculation, tubular cell death, tubulointerstitial nephritis and fibrosis. Genetic deletion of arginase-2 partially restores microcirculation and thereby alleviates tubular injury. We also demonstrate that BDL in mice is an excellent, clinically relevant model to study the renal consequences of HRS. (Hepatology 2018; 00:000-000).

Keyphrases

cell death
nitric oxide
high fat diet induced
nitric oxide synthase
type diabetes
endothelial cells
gene expression
high glucose
genome wide
dna methylation
adipose tissue
insulin resistance
signaling pathway
pi k akt
cell proliferation