Reactive oxygen species are involved in insulin-dependent regulation of autophagy in primary rat podocytes

• Podocytes injury underlies pathological changes in kidneys in diabetic nephropathy.
• Primary rat podocytes are characterized by a high level of basal autophagic activity.
• Insulin affects albumin permeability in cultured podocyte monolayers.
• Insulin induces autophagy in podocytes in an ROS-dependent manner.

Autophagy is an intracellular defense mechanism responsible for the turnover of damaged or non-functional cellular constituents. This process provides cells with energy and essential compounds under unfavorable environmental conditions—such as oxidative stress and hyperglycemia, which are both observed in diabetes. The most common diabetes complication is diabetic nephropathy (DN), which can lead to renal failure. This condition often includes impaired podocyte function. Here we investigated autophagic activity in rat podocytes cultured with a high insulin concentration (300 nM). Autophagy was activated after 60 min of insulin stimulation. Moreover, this effect was abolished following pharmacological (apocynin) or genetic (siRNA) inhibition of NAD(P)H oxidase activity, indicating that insulin-dependent autophagy stimulation involved reactive oxygen species (ROS). We also observed a continuous and time-dependent increase of podocyte albumin permeability in response to insulin, and this process was slightly improved by autophagy inhibition following short-term insulin exposure. Our results suggest that insulin may be a factor affecting the development of diabetic nephropathy.