PLoS ONE (Jan 2015)

Prion Protein Protects against Renal Ischemia/Reperfusion Injury.

  • Bo Zhang,
  • Daniel Cowden,
  • Fan Zhang,
  • Jue Yuan,
  • Sandra Siedlak,
  • Mai Abouelsaad,
  • Liang Zeng,
  • Xuefeng Zhou,
  • John O'Toole,
  • Alvin S Das,
  • Diane Kofskey,
  • Miriam Warren,
  • Zehua Bian,
  • Yuqi Cui,
  • Tao Tan,
  • Adam Kresak,
  • Robert E Wyza,
  • Robert B Petersen,
  • Gong-Xian Wang,
  • Qingzhong Kong,
  • Xinglong Wang,
  • John Sedor,
  • Xiongwei Zhu,
  • Hua Zhu,
  • Wen-Quan Zou

DOI
https://doi.org/10.1371/journal.pone.0136923
Journal volume & issue
Vol. 10, no. 9
p. e0136923

Abstract

Read online

The cellular prion protein (PrPC), a protein most noted for its link to prion diseases, has been found to play a protective role in ischemic brain injury. To investigate the role of PrPC in the kidney, an organ highly prone to ischemia/reperfusion (IR) injury, we examined wild-type (WT) and PrPC knockout (KO) mice that were subjected to 30-min of renal ischemia followed by 1, 2, or 3 days of reperfusion. Renal dysfunction and structural damage was more severe in KO than in WT mice. While PrP was undetectable in KO kidneys, Western blotting revealed an increase in PrP in IR-injured WT kidneys compared to sham-treated kidneys. Compared to WT, KO kidneys exhibited increases in oxidative stress markers heme oxygenase-1, nitrotyrosine, and Nε-(carboxymethyl)lysine, and decreases in mitochondrial complexes I and III. Notably, phosphorylated extracellular signal-regulated kinase (pERK) staining was predominantly observed in tubular cells from KO mice following 2 days of reperfusion, a time at which significant differences in renal dysfunction, histological changes, oxidative stress, and mitochondrial complexes between WT and KO mice were observed. Our study provides the first evidence that PrPC may play a protective role in renal IR injury, likely through its effects on mitochondria and ERK signaling pathways.