4.7 Article

Integrated regulation of stress responses, autophagy and survival by altered intracellular iron stores

REDOX BIOLOGY (2022)

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Journal

REDOX BIOLOGY
Volume 55, Issue -, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.redox.2022.102407

Keywords

ATF4; ER stress; Ferroptosis; Lipid peroxidation; Mitochondria

Categories

Biochemistry & Molecular Biology

Funding

  1. National Institute of Health [R01DK125647, R01DK044234]
  2. VA Research and Development Merit Review Award [BX000136-08]
  3. Emory University School of Medicine
  4. Emory College of Arts and Sciences
  5. Georgia Clinical & Translational Science Alliance

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Iron excess and deficiency can cause cellular stress and death through the common mechanism of impaired autophagic function.
Iron is a mineral essential for blood production and a variety of critical cellular functions. Altered iron meta-bolism has been increasingly observed in many diseases and disorders, but a comprehensive and mechanistic understanding of the cellular impact of impaired iron metabolism is still lacking. We examined the effects of iron overload or iron deficiency on cellular stress responses and autophagy which collectively regulate cell homeo-stasis and survival. Acute iron loading led to increased mitochondrial ROS (mtROS) production and damage, lipid peroxidation, impaired autophagic flux, and ferroptosis. Iron-induced mtROS overproduction is the mechanism of increased lipid peroxidation, impaired autophagy, and the induction of ferroptosis. Iron excess -induced ferroptosis was cell-type dependent and regulated by activating transcription factor 4 (ATF4). Upre-gulation of ATF4 mitigated iron-induced autophagic dysfunction and ferroptosis, whereas silencing of ATF4 expression impaired autophagy and resulted in increased mtROS production and ferroptosis. Employing autophagy-deficient hepatocytes and different autophagy inhibitors, we further showed that autophagic impairment sensitized cells to iron-induced ferroptosis. In contrast, iron deficiency activated the endoplasmic reticulum (ER) stress response, decreased autophagy, and induced apoptosis. Decreased autophagy associated with iron deficiency was due to ER stress, as reduction of ER stress by 4-phenylbutyric acid (4-PBA) improved autophagic flux. The mechanism of decreased autophagy in iron deficiency is a disruption in lysosomal biogenesis due to impaired posttranslational maturation of lysosomal membrane proteins. In conclusion, iron excess and iron deficiency cause different forms of cell stress and death in part through the common mechanism of impaired autophagic function.

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