Mitochondrial Aconitase Enzymatic Activity: A Potential Long-Term Survival Biomarker in the Blood of ALS Patients

Cristina González-Mingot; Francisco Javier Miana-Mena; Pedro José Iñarrea; Cristina Iñiguez; José Luis Capablo; Rosario Osta; Anna Gil-Sánchez; Luis Brieva; Pilar Larrodé

doi:10.3390/jcm12103560

Mitochondrial Aconitase Enzymatic Activity: A Potential Long-Term Survival Biomarker in the Blood of ALS Patients

J Clin Med. 2023 May 19;12(10):3560. doi: 10.3390/jcm12103560.

Authors

Cristina González-Mingot¹, Francisco Javier Miana-Mena², Pedro José Iñarrea³, Cristina Iñiguez⁴, José Luis Capablo⁵, Rosario Osta², Anna Gil-Sánchez¹, Luis Brieva¹, Pilar Larrodé⁴

Affiliations

¹ Neurology-Department, Hospital Arnau de Vilanova of Lleida, 25198 Lleida, Spain.
² LAGENBIO-Centro de Investigación Biomédica en Red de Enfermedades Neurodegenerativas (CIBERNED), Aragon Institute for Health Research (IIS Aragon), Zaragoza University, 50013 Zaragoza, Spain.
³ Biochemical-Department of Biology-Faculty, Zaragoza University, 50009 Zaragoza, Spain.
⁴ Neurology-Department, Hospital Clínico Universitario Lozano Blesa of Zaragoza, 50009 Zaragoza, Spain.
⁵ Neurology-Department, Hospital Universitario Miguel Servet of Zaragoza, 50009 Zaragoza, Spain.

Abstract

Background: Amyotrophic lateral sclerosis (ALS) is a multisystemic, progressive, neurodegenerative disorder. Despite it being generally fatal within a period of 2-4 years, it is highly heterogeneous; as a result, survival periods may vary greatly among individual patients. Biomarkers can serve as tools for diagnosis, prognosis, indicators of therapeutic response, and future therapeutics. Free-radical-dependent mitochondrial damage is believed to play a crucial role in neurodegeneration in ALS. Mitochondrial aconitase, which is also known as aconitase 2 (Aco2), is a key Krebs cycle enzyme and is involved in the regulation of cellular metabolism and iron homeostasis. Aco2 is very sensitive to oxidative inactivation and can aggregate and accumulate in the mitochondrial matrix, causing mitochondrial dysfunction. Loss of Aco2 activity may therefore reflect increased levels of mitochondrial dysfunction due to oxidative damage and could be relevant to ALS pathogenesis. The aim of our study was to confirm changes in mitochondrial aconitase activity in peripheral blood and to determine whether such changes are dependent on, or independent of, the patient's condition and to propose the feasibility of using them as possible valid biomarkers to quantify the progression of the disease and as a predictor of individual prognosis in ALS.

Methods: We measured the Aco2 enzymatic activity in the platelets of blood samples taken from 22 controls and 26 ALS patients at different stages of disease development. We then correlated antioxidant activity with clinical and prognostic variables.

Results: Aco2 activity was significantly lower in the 26 ALS patients than in the 22 controls (p < 0.05). Patients with higher levels of Aco2 activity survived longer than those with lower levels (p < 0.05). Aco2 activity was also higher in patients with earlier onset (p < 0.05) and in those with predominantly upper motor neuron signs.

Conclusions: Aco2 activity seems to be an independent factor that could be used in the long-term survival prognosis of ALS. Our findings suggest that blood Aco2 could be a leading candidate for use as a biomarker to improve prognosis. More studies are needed to confirm these results.

Keywords: ALS; aconitase; biomarker; enzymatic activity; mitochondrial antioxidant activity.

Grants and funding

This work has not received external funding.