Alternative pathways of programmed cell death are activated in cells with defective caspase-dependent apoptosis

• Authors: ONDROUŠKOVÁ Eva; SOUČEK Karel; HORVÁTH Viktor; ŠMARDA Jan
• Year of publication: 2008
• Type: Article in Periodical
• Magazine / Source: Leukemia Research
• MU Faculty or unit: Faculty of Science
• Field: Oncology and hematology
• Keywords: apoptosis; autophagy; programmed cell death
• Description: Loss of programmed cell death pathways is one of the features of malignancy that complicate the response of cancer cells to therapy. Activation of alternative death pathways offers a promising approach to enhance efficiency of cancer chemotherapy. We analysed programmed cell death pathways of v-myb-transformed BM2 monobolasts induced by arsenic trioxide, cycloheximide and camptothecin. We show that cell death is not executed by caspases but rather by alternative cell death pathways: camptothecin induces the lysosome-dependent cell death, arsenic trioxide induces autophagy, and most of cycloheximide-treated BM2 cells die by necrosis. The fact that alternative cell death pathways can be switched in cells with defects in activation and/or function of caspases suggests that understanding and targeting of these pathways could improve therapy on cancer cells suffering from defective apoptosis.

Related projects

• Molecular basis of cell and tissue regulations
• A role of certain transcription factors in the osteoclastic differentiation pathway