Abstract P212: Peroxiredoxin-4 And Dopamine D5 Receptor Interact To Reduce Oxidative Stress And Inflammation In The Kidney

Abstract

Peroxiredoxin-4 (PRDX4), an endoplasmic reticulum peroxiredoxin protein, plays a protective role against oxidative stress and inflammation by reducing hydrogen peroxide to water. The dopamine D5 receptor (D 5 R) is also important in protecting against oxidative stress, but the interaction between PRDX4 and D 5 R in regulating oxidative stress in the kidney is not known. In D 5 R-HEK 293 cells, fenoldopam (FEN, 25 nM/12 hr, n=4), a D1-likereceptor agonist, increased PRDX4 protein expression (1.92±0.12-fold over basal level, n=4), mainly in non-lipid rafts (LRs: 24.9±11.4%, non-LRs: 75.1±11.4%, baseline; LRs: 30.9±13.9%, non-LRs: 174.1±16.7%, FEN). FEN also increased the co-immunoprecipitation of D 5 R and PRDX4 and their colocalization, particularly in the endoplasmic reticulum. In human renal proximal tubule cells (hRPTCs), FEN (25 nM/12 hr, n=3) increased PRDX4 and D 5 R interaction in non-LRs, also. Si-RNA silencing of PRDX4 increased reactive oxygen species (ROS) production and impaired the inhibitory effect of FEN on ROS production (scrambled siRNA: 100.0±11.6% and 65.4±5.6% for Vehicle (Veh) and FEN, respectively; PRDX4 siRNA: 147.7±11.8% and 134.8±11.2% for Veh and FEN, respectively, n=4/group) detected by Amplex Red. In addition in both D 5 R-HEK 293 and hRPTCs, siRNA silencing of PRDX4 increased the production of interleukin-1β (26.88±3.8 and 46.40±4.2 pg/mL [n=3, D 5 R-HEK 293]; 15.87±1.2 and 37.9±1.4 pg/mL [n=3 in hRPTCs]), tumor necrosis factor (131.7±6.5 and 271.2±18.1 pg/mL [n=4, D 5 R-HEK 293]; 108.8±11.8 and 240.1±13.7 pg/mL [n=4 in hRPTCs]), and caspase-12 (15.21±3.8 and 40.78±4.3 ng/mL [n=4,n D 5 R-HEK 293]; 8.8±1.1 and 27.9±2.0 ng/mL [n=4, hRPTCs]). Furthermore, the protein expression of D 5 R was decreased in PRDX4 siRNA-treated D 5 R-HEK293 (~41.2%, n=3) and hRPTCs (~39.6%, n=3). PRDX4 protein was also reduced in the kidney homogenates from D 5 R -/- mice (WT: 1.00±0.18, n=5; D 5 R -/- : 0.686±0.14, n=4; P<0.05). Taken together, PRDX4 interacts with D 5 R to decrease oxidative stress and inflammation in the kidney.