4.6 Editorial Material

ESCRT-III-mediated membrane repair in cell death and tumor resistance

Journal

CANCER GENE THERAPY
Volume 28, Issue 1-2, Pages 1-4

Publisher

SPRINGERNATURE
DOI: 10.1038/s41417-020-0200-0

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Funding

  1. US National Institutes of Health [R01CA229275]
  2. American Cancer Society [RSG-16-014-01-CDD]

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The plasma membrane acts as a barrier and gatekeeper under physiological conditions to protect cells, but undergoes structural and functional changes in pathological situations leading to cell damage. ESCRT-III plays a key role in repairing damaged plasma membranes during various types of regulated cell death, suggesting it as a potential target for overcoming drug resistance in tumor therapy.
The plasma membrane is made of glycerophospholipids that separate the inner and outer parts of the cell. Under physiological conditions, it acts as a barrier and gatekeeper to protect cells from the environment. In pathological situations, it undergoes structural and functional changes, resulting in cell damage. Indeed, plasma membrane damage caused by various stresses (e.g., hypoxia, nutritional deficiencies, ultraviolet radiation, and chemotherapeutic agents) is one of the hallmarks of cell death. Phosphatidylserine exposure and plasma membrane blebbing usually occurs in apoptotic cells, while necrotic cells lose the integrity of the plasma membrane and thereby release intracellular damage-associated molecular patterns. In contrast, the endosomal sorting complex required for transport-III (ESCRT-III), an evolutionarily conserved protein complex with membrane fission machinery, plays a key role in the repair of damaged plasma membranes in various types of regulated cell death, such as necroptosis, pyroptosis, and ferroptosis. These emerging findings indicate that ESCRT-III is a potential target to overcome drug resistance during tumor therapy.

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