ALDH2/eIF3E Interaction Modulates Protein Translation Critical for Cardiomyocyte Ferroptosis in Acute Myocardial Ischemia Injury

Oct 20, 2025Circulation

Interaction Between ALDH2 and eIF3E Controls Protein Production Linked to Heart Cell Death in Acute Heart Attack

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Abstract

Carriers of the ALDH22 variant experience more severe heart failure* after acute myocardial infarction (AMI).

  • ALDH2*2 is linked to increased lipid peroxidation and decreased antioxidant levels in patients after AMI.
  • In mouse models, ALDH2*2 displays similar features of ferroptosis, indicating a potential mechanism for heart injury.
  • Ferroptosis inhibition in these models improved heart function and reversed markers associated with ferroptosis.
  • The ALDH2*2 variant reduces ALDH2 protein levels and increases the expression of ferroptosis-related markers in heart tissues.
  • ALDH2 interacts with the eIF3 complex, and the ALDH2*2 variant disrupts this interaction, leading to enhanced translation of certain mRNAs that promote ferroptosis.

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