MPO/HOCl Facilitates Apoptosis and Ferroptosis in the SOD1 Motor Neuron of Amyotrophic Lateral Sclerosis.

BACKGROUND

Oxidative stress and reactive oxygen species (ROS) are important in the pathogenesis of amyotrophic lateral sclerosis (ALS). Hypochlorous acid (HOCl) is a powerful oxidant of the reactive oxygen species (ROS) family. HOCl's role in the progress of ALS remains unclear due to the lack of an effective HOCl detection method. Cumulative evidence supports oxidative damage incurred by mutant hSOD1 contributing to motor neuron death; however, whether HOCl as well as its catalytic enzyme myeloperoxidase (MPO) function in the cell death of SOD1 ALS remains elusive.

METHODS

The hSOD1 and hSOD1 NSC-34 cell and SOD1 ALS mouse models were employed. With a novel fluorescent HOCl probe, HKOCl-3, we detected the expressions of HOCl and its catalytic enzyme, MPO, in the above models and . The regulation of MPO/HOCl by hSOD1 mutation and cell deaths by MPO/HOCl were also assayed, including apoptosis, ferroptosis, and autophagy.

RESULTS

Our results showed that hSOD1 mutation promoted the activation of the MPO/HOCl pathway in SOD1 ALS cell models. The activation of MPO/HOCl pathways facilitated apoptosis and ferroptosis through increasing the Bax/Bcl-2 ratio and expression of caspase-3 or inhibiting the expressions of GPX4 and NQO1 and thus leading to irreversible lipid peroxidation. Overexpressed FSP1, a glutathione-independent suppressor, could ameliorate ferroptosis. , we demonstrated that the activation of the MPO/HOCl pathway occurred differently in motor neurons of the motor cortices, brain stems, and spinal cords in male and female SOD1 transgenic mice. In addition, inhibiting MPO improved the motor performance of SOD1 transgenic mice, as demonstrated by the rotarod test.

CONCLUSIONS

We concluded that aggregation of mutant hSOD1 proteins contributed to activation of the MPO/HOCl pathway, triggering apoptosis and ferroptosis in motor neuronal deaths and exerting impaired motor performance.