Cytochrome C is Released from Mitochondria in a Reactive Oxygen Species (ROS)-dependent Fashion and Can Operate As a ROS Scavenger and As a Respiratory Substrate in Cerebellar Neurons Undergoing Excitotoxic Death

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2000 Sep 12

PMID 10980192

Citations 67

Authors

A Atlante

P Calissano

A Bobba

A Azzariti

E Marra

S Passarella

Affiliations

Soon will be listed here.

Abstract

In rat cerebellar granule cells both reactive oxygen species production and release of cytochrome c take place during glutamate toxicity. This investigation was aimed (i) to ascertain whether and how these two processes are related and (ii) to gain insight into the role played by the released cytochrome c in the onset of neurotoxicity. Cytochrome c release takes place owing to the generation of reactive oxygen species both in glutamate-treated cerebellar granule cells and in sister control cultures incubated in the presence of the reactive oxygen species-generating system consisting of xanthine plus xanthine oxidase. In the early phase of neurotoxicity (30-min glutamate exposure) about 40% of the maximum (as measured at 3 h of glutamate exposure) cytochrome c release was found to occur in cerebellar granule cells from mitochondria that were essentially coupled and intact and that had a negligible production of oxygen free radicals. Contrarily, mitochondria from cells treated with glutamate for 3 h were mostly uncoupled and produced reactive oxygen species at a high rate. The cytosolic fraction containing the released cytochrome c was able to transfer electrons from superoxide anion to molecular oxygen via the respiratory chain and was found to partially prevent glutamate toxicity when added externally to cerebellar neurons undergoing necrosis. In the light of these findings, we propose that in the early phase of neurotoxicity, cytochrome c release can be part of a cellular and mitochondrial defense mechanism against oxidative stress.

Citing Articles

Order-to-Disorder and Disorder-to-Order Transitions of Proteins upon Binding to Phospholipid Membranes: Common Ground and Dissimilarities.

Schweitzer-Stenner R Biomolecules. 2025; 15(2).

PMID: 40001501 PMC: 11852466. DOI: 10.3390/biom15020198.

Genetic variation in CCDC93 is associated with elevated central systolic blood pressure, impaired arterial relaxation, and mitochondrial dysfunction.

Kumar N, Yang M, Sun P, Hunker K, Li J, Jia J PLoS Genet. 2024; 20(9):e1011151.

PMID: 39250516 PMC: 11421807. DOI: 10.1371/journal.pgen.1011151.

Socialized mitochondria: mitonuclear crosstalk in stress.

Kim K, Lee C Exp Mol Med. 2024; 56(5):1033-1042.

PMID: 38689084 PMC: 11148012. DOI: 10.1038/s12276-024-01211-4.

Targeted Delivery of Geraniol via Hyaluronic Acid-Conjugation Enhances Its Anti-Tumor Activity Against Prostate Cancer.

Yu H, Ning N, He F, Xu J, Zhao H, Duan S Int J Nanomedicine. 2024; 19:155-169.

PMID: 38204602 PMC: 10778230. DOI: 10.2147/IJN.S444815.

Mitochondrial Metabolism: A New Dimension of Personalized Oncology.

Behnam B, Taghizadeh-Hesary F Cancers (Basel). 2023; 15(16).

PMID: 37627086 PMC: 10452105. DOI: 10.3390/cancers15164058.