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Critical involvement of lysyl oxidase in seizure-induced neuronal damage through ERK-Alox5-dependent ferroptosis and its therapeutic implications

Xiao‐Yuan Mao, Xuan Wang, Mingzhu Jin, Qin Li, Ji-Ning Jia, Menghuan Li, Hong‐Hao Zhou, Zhaoqian Liu, Weilin Jin, Yanli Zhao, Zhong Luo

2022Acta Pharmaceutica Sinica B43 citationsDOIOpen Access PDF

Abstract

Recent insights collectively suggest the important roles of lysyl oxidase (LysOX) in the pathological processes of several acute and chronic neurological diseases, but the molecular regulatory mechanisms remain elusive. Herein, we explore the regulatory role of LysOX in the seizure-induced ferroptotic cell death of neurons. Mechanistically, LysOX promotes ferroptosis-associated lipid peroxidation in neurons via activating extracellular regulated protein kinase (ERK)-dependent 5-lipoxygenase (Alox5) signaling. In addition, overexpression of LysOX via adeno-associated viral vector (AAV)-based gene transfer enhances ferroptosis sensitivity and aggravates seizure-induced hippocampal damage. Our studies show that pharmacological inhibition of LysOX with β-aminopropionitrile (BAPN) significantly blocks seizure-induced ferroptosis and thereby alleviates neuronal damage, while the BAPN-associated cardiotoxicity and neurotoxicity could further be reduced through encapsulation with bioresponsive amorphous calcium carbonate-based nanocarriers. These findings unveil a previously unrecognized LysOX-ERK-Alox5 pathway for ferroptosis regulation during seizure-induced neuronal damage. Suppressing this pathway may yield therapeutic implications for restoring seizure-induced neuronal injury.

Topics & Concepts

MAPK/ERK pathwayLipid peroxidationNADPH oxidaseLysyl oxidaseProgrammed cell deathCell biologyChemistryKinaseEpilepsyPharmacologyNeuroscienceBiologyOxidative stressReactive oxygen speciesBiochemistryApoptosisExtracellular matrixMicrobial metabolism and enzyme functionEicosanoids and Hypertension PharmacologyMacrophage Migration Inhibitory Factor