Reversible Thiol Oxidation Increases Mitochondrial Electron Transport Complex Enzyme Activity but Not Respiration in Cardiomyocytes from Patients with End-Stage Heart Failure.
Ravi A KumarTrace ThomeOmar M SharafTerence E RyanGeorge J ArnaoutakisEric I JengLeonardo F FerreiraPublished in: Cells (2022)
Cardiomyocyte dysfunction in patients with end-stage heart failure with reduced ejection fraction (HFrEF) stems from mitochondrial dysfunction, which contributes to an energetic crisis. Mitochondrial dysfunction reportedly relates to increased markers of oxidative stress, but the impact of reversible thiol oxidation on myocardial mitochondrial function in patients with HFrEF has not been investigated. In the present study, we assessed mitochondrial function in ventricular biopsies from patients with end-stage HFrEF in the presence and absence of the thiol-reducing agent dithiothreitol (DTT). Isolated mitochondria exposed to DTT had increased enzyme activity of complexes I ( p = 0.009) and III ( p = 0.018) of the electron transport system, while complexes II ( p = 0.630) and IV ( p = 0.926) showed no changes. However, increased enzyme activity did not carry over to measurements of mitochondrial respiration in permeabilized bundles. Oxidative phosphorylation conductance ( p = 0.439), maximal respiration ( p = 0.312), and ADP sensitivity ( p = 0.514) were unchanged by 5 mM DTT treatment. These results indicate that mitochondrial function can be modulated through reversible thiol oxidation, but other components of mitochondrial energy transfer are rate limiting in end-stage HFrEF. Optimal therapies to normalize cardiac mitochondrial respiration in patients with end-stage HFrEF may benefit from interventions to reverse thiol oxidation, which limits complex I and III activities.
Keyphrases
- oxidative stress
- heart failure
- left ventricular
- hydrogen peroxide
- electron transfer
- energy transfer
- dna damage
- induced apoptosis
- ischemia reperfusion injury
- diabetic rats
- public health
- physical activity
- cardiac resynchronization therapy
- quantum dots
- heart rate
- angiotensin ii
- endoplasmic reticulum stress
- ultrasound guided
- high resolution
- resistance training
- signaling pathway
- catheter ablation
- heat shock protein