Reviewing the Role of Mitochondrial Dysfunction in Alzheimer's Disease

Mitochondria are the powerhouses of neurons, supplying the ATP needed for synaptic transmission and plasticity. In Alzheimer’s disease, post‑mortem studies reveal smaller organelles, broken cristae, and depleted mitochondrial DNA, all of which compromise oxidative phosphorylation. The mitochondrial cascade hypothesis positions these bioenergetic failures as upstream events that trigger amyloid‑beta accumulation and tau hyperphosphorylation, reframing AD as a metabolic disorder rather than solely a protein‑aggregation disease.

Therapeutic interest has shifted toward restoring mitochondrial function directly. Mitochondrial transplantation—isolating healthy organelles from cultured cells and delivering them into the cerebrospinal fluid—has demonstrated sustained ATP recovery and cognitive benefits in rodent models of neurodegeneration. Intrathecal administration bypasses the blood‑brain barrier, yet the approach must contend with age‑related vascular insufficiency that limits oxygen and glucose delivery to transplanted mitochondria. Optimizing delivery vectors and pairing transplantation with vascular health interventions could amplify therapeutic impact.

The implications extend beyond Alzheimer’s, as mitochondrial deficits are common across neurodegenerative disorders. Rigorous clinical trials are needed to validate safety, dosing, and long‑term efficacy, while biomarkers such as cerebrospinal fluid mtDNA levels may guide patient selection. Success could spawn a new class of metabolic therapeutics, attracting biotech investment and reshaping treatment paradigms for aging‑related brain diseases.