PLoS ONE (Jan 2018)

ALG-2 participates in recovery of cells after plasma membrane damage by electroporation and digitonin treatment.

  • Jonas M la Cour,
  • Pernille Winding Gojkovic,
  • Sophie E B Ambjørner,
  • Jonas Bagge,
  • Simone M Jensen,
  • Svetlana Panina,
  • Martin W Berchtold

DOI
https://doi.org/10.1371/journal.pone.0204520
Journal volume & issue
Vol. 13, no. 9
p. e0204520

Abstract

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The calcium binding protein ALG-2 is upregulated in several types of cancerous tissues and cancer cell death may be a consequence of ALG-2 downregulation. Novel research suggests that ALG-2 is involved in membrane repair mechanisms, in line with several published studies linking ALG-2 to processes of membrane remodeling and transport, which may contribute to the fitness of cells or protect them from damage. To investigate the involvement of ALG-2 in cell recovery after membrane damage we disrupted the PDCD6 gene encoding the ALG-2 protein in DT-40 cells and exposed them to electroporation. ALG-2 knock-out cells were more sensitive to electroporation as compared to wild type cells. This phenotype could be reversed by reestablishing ALG-2 expression confirming that ALG-2 plays an important role in cell recovery after plasma membrane damage. We found that overexpression of wild type ALG-2 but not a mutated form unable to bind Ca2+ partially protected HeLa cells from digitonin-induced cell death. Further, we were able to inhibit the cell protective function of ALG-2 after digitonin treatment by adding a peptide with the ALG-2 binding sequence of ALIX, which has been proposed to serve as the ALG-2 downstream target in a number of processes including cell membrane repair. Our results suggest that ALG-2 may serve as a novel therapeutic target in combination with membrane damaging interventions.