The β2-adrenergic receptor agonist formoterol restores mitochondrial homeostasis in glucose-induced renal proximal tubule injury through separate integrated pathways

Kristan H Cleveland; Rick G Schnellmann

doi:10.1016/j.bcp.2023.115436

The β₂-adrenergic receptor agonist formoterol restores mitochondrial homeostasis in glucose-induced renal proximal tubule injury through separate integrated pathways

Biochem Pharmacol. 2023 Mar:209:115436. doi: 10.1016/j.bcp.2023.115436. Epub 2023 Jan 30.

Authors

Kristan H Cleveland¹, Rick G Schnellmann²

Affiliations

¹ Department of Pharmacology and Toxicology, College of Pharmacy, University of Arizona, Tucson, AZ, United States.
² Department of Pharmacology and Toxicology, College of Pharmacy, University of Arizona, Tucson, AZ, United States; Southern Arizona VA Health Care System, Tucson, AZ, United States; Southwest Environmental Health Science Center, University of Arizona, Tucson, AZ, United States. Electronic address: schnell@pharmacy.arizona.edu.

PMID: 36720358
DOI: 10.1016/j.bcp.2023.115436

Abstract

Mitochondrial dysfunction drives the development and progression of diabetic kidney disease (DKD). Previously, we discovered that the β₂-adrenergic receptor (AR) agonist formoterol regulates mitochondrial dynamics in the hyperglycemic renal proximal tubule. The goal of this study was to identify signaling mechanisms through which formoterol restores the mitochondrial fission/fusion proteins Drp1 and Mfn1. Using primary renal proximal tubule cells (RPTC), the effect of chronic high glucose on RhoA/ROCK1/Drp1 and Raf/MEK1/2/ERK1/2/Mfn1 signaling was determined. In glucose-treated RPTC, RhoA became hyperactive, leading to ROCK1-induced activation of Drp1. Treatment with formoterol and/or pharmacological inhibitors targeting RhoA, ROCK1 and Drp1 blocked RhoA and Drp1 hyperactivity. Inhibiting this pathway also restored maximal mitochondrial respiration. By preventing Gβγ signaling with gallein, we determined that formoterol signals through the Gβγ subunit of the β₂-AR to restore RhoA and Drp1. Furthermore, formoterol restored this pathway by blocking binding of RhoA with the guanine nucleotide exchange factor p114RhoGEF. Formoterol also restored the mitochondrial fusion protein Mfn1 through a second Gβγ-dependent mechanism composed of Raf/MEK1/2/ERK1/2/Mfn1. Glucose-treated RPTC exhibited decreased Mfn1 activity, which was restored with formoterol. Pharmacological inhibition of Gβγ, Raf and MEK1/2 also restored Mfn1 activity. We demonstrate that glucose promotes the interaction between RhoA and p114RhoGEF, leading to increased RhoA and ROCK1-mediated activation of Drp1, and decreases Mfn1 activity through Raf/MEK1/2/ERK1/2. Formoterol restores these pathways and mitochondrial function in response to elevated glucose by activating separate yet integrative pathways that promote mitochondrial biogenesis, decreased fission and increased fusion in RPTC, further supporting its potential as a therapeutic for DKD.

Keywords: Diabetic kidney disease (DKD); Formoterol; Mitochondria; Renal proximal tubule; β(2)-adrenergic receptor.

Publication types

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

MeSH terms

Adrenergic Agonists / metabolism
Dynamins / metabolism
Formoterol Fumarate / metabolism
Glucose* / metabolism
Homeostasis
Mitochondria* / metabolism
Mitochondrial Dynamics

Substances

Formoterol Fumarate
Glucose
Adrenergic Agonists
Dynamins