Researchers from the University of Osaka have demonstrated that mitochondrial hyperfusion, when induced by low levels of DRP1 or cellular stress, activates an immune response through the RIG-I–MAVS pathway. Dependent on the involvement of the BAX protein, the release of mitochondrial RNA into the cytosol enhanced natural killer cell cytotoxicity and reduced tumor growth in a xenograft model. The findings, published in Cell Reports, provide new possibilities for cancer research and treatment.
Mitochondria are constantly dividing and fusing within our cells, reshaping themselves to keep up with the cell’s changing needs. Sometimes, though, things go awry, and mitochondria can grow abnormally long. Are these long mitochondria harmful, or might they serve a purpose?
Mitochondria also act as signaling centers, helping the cell sense and respond to trouble. When mitochondria are hyperfused, for example in the stressed, abnormally long state described above, they release their genetic material into the cytosol, where the cell treats it as a warning sign in the same way it would treat a virus.
