Antioxidants (Apr 2022)

Paraoxonase-1 Regulation of Renal Inflammation and Fibrosis in Chronic Kidney Disease

  • Fatimah K. Khalaf,
  • Chrysan J. Mohammed,
  • Prabhatchandra Dube,
  • Jacob A. Connolly,
  • Apurva Lad,
  • Usman M. Ashraf,
  • Joshua D. Breidenbach,
  • Robin C. Su,
  • Andrew L. Kleinhenz,
  • Deepak Malhotra,
  • Amira F. Gohara,
  • Steven T. Haller,
  • David J. Kennedy

DOI
https://doi.org/10.3390/antiox11050900
Journal volume & issue
Vol. 11, no. 5
p. 900

Abstract

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Papraoxonase-1 (PON1) is a hydrolytic lactonase enzyme that is synthesized in the liver and circulates attached to high-density lipoproteins (HDL). Clinical studies have demonstrated an association between diminished PON-1 and the progression of chronic kidney disease (CKD). However, whether decreased PON-1 is mechanistically linked to renal injury is unknown. We tested the hypothesis that the absence of PON-1 is mechanistically linked to the progression of renal inflammation and injury in CKD. Experiments were performed on control Dahl salt-sensitive rats (SSMcwi, hereafter designated SS rats) and Pon1 knock-out rats (designated SS-Pon1em1Mcwi, hereafter designated SS-PON-1 KO rats) generated by injecting a CRISPR targeting the sequence into SSMcwi rat embryos. The resulting mutation is a 7 bp frameshift insertion in exon 4 of the PON-1 gene. First, to examine the renal protective role of PON-1 in settings of CKD, ten-week-old, age-matched male rats were maintained on a high-salt diet (8% NaCl) for up to 5 weeks to initiate the salt-sensitive hypertensive renal disease characteristic of this model. We found that SS-PON-1 KO rats demonstrated several hallmarks of increased renal injury vs. SS rats including increased renal fibrosis, sclerosis, and tubular injury. SS-PON-1 KO also demonstrated increased recruitment of immune cells in the renal interstitium, as well as increased expression of inflammatory genes compared to SS rats (all p p < 0.05) decline in renal function and increased renal oxidative stress compared to SS rats, despite no differences in blood pressure between the two groups. These findings suggest a new role for PON-1 in regulating renal inflammation and fibrosis in the setting of chronic renal disease independent of blood pressure.

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