Frataxin and Parkinson's disease (PD) are connected through mitochondrial dysfunction, oxidative stress, and iron homeostasis, which are common pathological features of both conditions. Here's how they relate:
1. Frataxin's Role in Mitochondrial Function and Iron Homeostasis
Frataxin is a mitochondrial protein primarily involved in:
- Iron storage and regulation: It helps in forming iron-sulfur clusters (ISC), essential for mitochondrial enzymes.
- Protecting against oxidative stress: Frataxin limits free iron accumulation, which can catalyze the production of reactive oxygen species (ROS) through the Fenton reaction.
In Friedreich's ataxia, frataxin deficiency leads to mitochondrial iron accumulation, increased ROS production, and subsequent oxidative damage.
2. Parkinson's Disease and Mitochondrial Dysfunction
PD is characterized by:
- Loss of dopaminergic neurons: This loss occurs in the substantia nigra, partly due to oxidative stress and mitochondrial dysfunction.
- Iron accumulation in the brain: Elevated iron levels are often found in the substantia nigra of PD patients, exacerbating oxidative damage.
3. Shared Mechanisms Between Frataxin Deficiency and PD
- Mitochondrial Dysfunction: Both conditions exhibit impaired mitochondrial function and reduced activity of iron-sulfur cluster-dependent enzymes.
- Oxidative Stress: Frataxin deficiency and PD share a tendency for increased oxidative stress, driven by dysregulated iron metabolism.
- Iron Dysregulation: Abnormal iron accumulation is a hallmark in both disorders, contributing to neurodegeneration.
4. Potential Links in Pathogenesis
- Common Pathways: Research suggests that frataxin dysregulation may play a role in PD-like pathology. Deficient frataxin activity could exacerbate mitochondrial impairments and oxidative stress seen in PD.
- Therapeutic Targets: Therapies aimed at modulating iron metabolism, enhancing mitochondrial function, or reducing oxidative stress are being explored in both Friedreich's ataxia and PD.
While frataxin is not the primary protein implicated in PD (unlike α-synuclein), the overlap in mitochondrial and iron-related mechanisms highlights a potential area for deeper investigation into their connection and shared therapeutic approaches.
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