TY - JOUR
T1 - Mitochondrion-Mediated Cell Death through Erk1-Alox5 Independent of Caspase-9 Signaling
AU - Chen, Min
AU - Wang, Lei
AU - Li, Min
AU - Budai, Marietta M.
AU - Wang, Jin
N1 - Funding Information:
This work was supported by grants from the US NIH grants: R01GM087710 (J.W.), R01AI123221 (J.W.) and R01DK083164 (M.C.). This work was also supported by grant from United States Department of Defense: PR190958 (M.C.). Flow cytometry and cell sorting for this project was supported by the Cytometry and Cell Sorting Core at Baylor College of Medicine and the Methodist Hospital Research Institute with funding from the NIH (P30 AI036211, P30 CA125123, and S10 RR024574).
Publisher Copyright:
© 2022 by the authors.
PY - 2022/10
Y1 - 2022/10
N2 - Mitochondrial disruption leads to the release of cytochrome c to activate caspase-9 and the downstream caspase cascade for the execution of apoptosis. However, cell death can proceed efficiently in the absence of caspase-9 following mitochondrial disruption, suggesting the existence of caspase-9-independent cell death mechanisms. Through a genome-wide siRNA library screening, we identified a network of genes that mediate caspase-9-independent cell death, through ROS production and Alox5-dependent membrane lipid peroxidation. Erk1-dependent phosphorylation of Alox5 is critical for targeting Alox5 to the nuclear membrane to mediate lipid peroxidation, resulting in nuclear translocation of cytolytic molecules to induce DNA damage and cell death. Consistently, double knockouts of caspase-9 and Alox5 in mice, but not deletion of either gene alone, led to significant T cell expansion with inhibited cell death, indicating that caspase-9- and Alox5-dependent pathways function in parallel to regulate T cell death in vivo. This unbiased whole-genome screening reveals an Erk1-Alox5-mediated pathway that promotes membrane lipid peroxidation and nuclear translocation of cytolytic molecules, leading to the execution of cell death in parallel to the caspase-9 signaling cascade.
AB - Mitochondrial disruption leads to the release of cytochrome c to activate caspase-9 and the downstream caspase cascade for the execution of apoptosis. However, cell death can proceed efficiently in the absence of caspase-9 following mitochondrial disruption, suggesting the existence of caspase-9-independent cell death mechanisms. Through a genome-wide siRNA library screening, we identified a network of genes that mediate caspase-9-independent cell death, through ROS production and Alox5-dependent membrane lipid peroxidation. Erk1-dependent phosphorylation of Alox5 is critical for targeting Alox5 to the nuclear membrane to mediate lipid peroxidation, resulting in nuclear translocation of cytolytic molecules to induce DNA damage and cell death. Consistently, double knockouts of caspase-9 and Alox5 in mice, but not deletion of either gene alone, led to significant T cell expansion with inhibited cell death, indicating that caspase-9- and Alox5-dependent pathways function in parallel to regulate T cell death in vivo. This unbiased whole-genome screening reveals an Erk1-Alox5-mediated pathway that promotes membrane lipid peroxidation and nuclear translocation of cytolytic molecules, leading to the execution of cell death in parallel to the caspase-9 signaling cascade.
KW - Alox5
KW - Erk1
KW - ROS
KW - caspase-9-independent cell death
KW - lipid peroxidation
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U2 - 10.3390/cells11193053
DO - 10.3390/cells11193053
M3 - Article
AN - SCOPUS:85139791192
VL - 11
JO - Cells
JF - Cells
SN - 2073-4409
IS - 19
M1 - 3053
ER -