High glucose repatterns human podocyte energy metabolism during differentiation and diabetic nephropathy

Toshiyuki Imasawa; Emilie Obre; Nadège Bellance; Julie Lavie; Tomoko Imasawa; Claire Rigothier; Yahsou Delmas; Christian Combe; Didier Lacombe; Giovanni Benard; Stéphane Claverol; Marc Bonneu; Rodrigue Rossignol

doi:10.1096/fj.201600293R

High glucose repatterns human podocyte energy metabolism during differentiation and diabetic nephropathy

FASEB J. 2017 Jan;31(1):294-307. doi: 10.1096/fj.201600293R. Epub 2016 Oct 17.

Authors

Affiliations

¹ Kidney Center, National Hospital Organization Chiba-East Hospital, Chiba, Japan; imasawa@cehpnet.com.
² INSERM Unité 1211, Laboratory of Rare Diseases, Metabolism, and Genetics, Bordeaux University, Bordeaux, France.
³ Cellomet, Centre Hospitalier Universitaire Pellegrin, Bordeaux, France.
⁴ Department of Nephrology, Transplantation, and Dialysis, Bordeaux University Hospital Center, Bordeaux, France; and.
⁵ Center of Functional Genomics, Bordeaux University, Bordeaux, France.

Abstract

Podocytes play a key role in diabetic nephropathy pathogenesis, but alteration of their metabolism remains unknown in human kidney. By using a conditionally differentiating human podocyte cell line, we addressed the functional and molecular changes in podocyte energetics during in vitro development or under high glucose conditions. In 5 mM glucose medium, we observed a stepwise activation of oxidative metabolism during cell differentiation that was characterized by peroxisome proliferator-activated receptor-γ coactivator 1α (PGC-1α)-dependent stimulation of mitochondrial biogenesis and function, with concomitant reduction of the glycolytic enzyme content. Conversely, when podocytes were cultured in high glucose (20 mM), stepwise oxidative phosphorylation biogenesis was aborted, and a glycolytic switch occurred, with consecutive lactic acidosis. Expression of the master regulators of oxidative metabolism transcription factor A mitochondrial, PGC-1α, AMPK, and serine-threonine liver kinase B1 was altered by high glucose, as well as their downstream signaling networks. Focused transcriptomics revealed that myocyte-specific enhancer factor 2C (MEF2C) and myogenic factor 5 (MYF5) expression was inhibited by high glucose levels, and endoribonuclease-prepared small interfering RNA-mediated combined inhibition of those transcription factors phenocopied the glycolytic shift that was observed in high glucose conditions. Accordingly, a reduced expression of MEF2C, MYF5, and PGC-1α was found in kidney tissue sections that were obtained from patients with diabetic nephropathy. These findings obtained in human samples demonstrate that MEF2C-MYF5-dependent bioenergetic dedifferentiation occurs in podocytes that are confronted with a high-glucose milieu.-Imasawa, T., Obre, E., Bellance, N., Lavie, J., Imasawa, T., Rigothier, C., Delmas, Y., Combe, C., Lacombe, D., Benard, G., Claverol, S., Bonneu, M., Rossignol, R. High glucose repatterns human podocyte energy metabolism during differentiation and diabetic nephropathy.

Keywords: MEF2C; human kidney; mitochondria.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Bowman Capsule / metabolism
Cell Differentiation / drug effects*
Cells, Cultured
Diabetic Nephropathies / pathology*
Energy Metabolism / drug effects*
Energy Metabolism / physiology
Gene Expression Regulation
Glucose / administration & dosage
Glucose / pharmacology*
Humans
Oxidation-Reduction
Podocytes / drug effects*
Podocytes / physiology

Substances

Glucose