Oxidized alkyl phospholipids stimulate sodium transport in proximal tubules via a nongenomic PPARγ-dependent pathway

Tomohito Mizuno; Nobuhiko Satoh; Shoko Horita; Hiroyuki Tsukada; Mayuko Takagi; Yusuke Sato; Haruki Kume; Masaomi Nangaku; Motonobu Nakamura

doi:10.1016/j.jbc.2022.101681

Oxidized alkyl phospholipids stimulate sodium transport in proximal tubules via a nongenomic PPARγ-dependent pathway

J Biol Chem. 2022 Mar;298(3):101681. doi: 10.1016/j.jbc.2022.101681. Epub 2022 Feb 3.

Authors

Tomohito Mizuno¹, Nobuhiko Satoh¹, Shoko Horita¹, Hiroyuki Tsukada¹, Mayuko Takagi¹, Yusuke Sato², Haruki Kume², Masaomi Nangaku¹, Motonobu Nakamura³

Affiliations

¹ Division of Nephrology and Endocrinology, The University of Tokyo, Tokyo, Japan.
² Department of Urology, The University of Tokyo, Tokyo, Japan.
³ Division of Nephrology and Endocrinology, The University of Tokyo, Tokyo, Japan. Electronic address: nakamura-stm@umin.ac.jp.

Abstract

Oxidized phospholipids have been shown to exhibit pleiotropic effects in numerous biological contexts. For example, 1-O-hexadecyl-2-azelaoyl-sn-glycero-3-phosphocholine (azPC), an oxidized phospholipid formed from alkyl phosphatidylcholines, is a peroxisome proliferator-activated receptor gamma (PPARγ) nuclear receptor agonist. Although it has been reported that PPARγ agonists including thiazolidinediones can induce plasma volume expansion by enhancing renal sodium and water retention, the role of azPC in renal transport functions is unknown. In the present study, we investigated the effect of azPC on renal proximal tubule (PT) transport using isolated PTs and kidney cortex tissues and also investigated the effect of azPC on renal sodium handling in vivo. We showed using a microperfusion technique that azPC rapidly stimulated Na⁺/HCO₃^- cotransporter 1 (NBCe1) and luminal Na⁺/H⁺ exchanger (NHE) activities in a dose-dependent manner at submicromolar concentrations in isolated PTs from rats and humans. The rapid effects (within a few minutes) suggest that azPC activates NBCe1 and NHE via nongenomic signaling. The stimulatory effects were completely blocked by specific PPARγ antagonist GW9662, ERK kinase inhibitor PD98059, and CD36 inhibitor sulfosuccinimidyl oleate. Treatment with an siRNA against PPAR gamma completely blocked the stimulation of both NBCe1 and NHE by azPC. Moreover, azPC induced ERK phosphorylation in rat and human kidney cortex tissues, which were completely suppressed by GW9662 and PD98059 treatments. These results suggest that azPC stimulates renal PT sodium-coupled bicarbonate transport via a CD36/PPARγ/mitogen-activated protein/ERK kinase/ERK pathway. We conclude that the stimulatory effects of azPC on PT transport may be partially involved in volume expansion.

Keywords: Na(+)/H(+) exchanger; Na(+)/HCO(3)(−) cotransporter 1; kidney; oxidative stress; oxidized phospholipid; peroxisome proliferator–activated receptor; phospholipid; proximal tubule; sodium transport; sodium–proton exchange.

MeSH terms

Animals
CD36 Antigens / antagonists & inhibitors
CD36 Antigens / metabolism
Hypoglycemic Agents / pharmacology
Kidney Tubules, Proximal* / drug effects
Kidney Tubules, Proximal* / metabolism
Oxidation-Reduction
PPAR gamma* / metabolism
Phospholipids* / metabolism
Rats
Signal Transduction
Sodium-Hydrogen Exchangers* / metabolism
Thiazolidinediones / pharmacology

Substances

CD36 Antigens
Hypoglycemic Agents
PPAR gamma
Phospholipids
Sodium-Hydrogen Exchangers
Thiazolidinediones