Regulation of an ATG7-beclin 1 Program of Autophagic Cell Death by Caspase-8

L Yu, A Alva, H Su, P Dutt, E Freundt, S Welsh… - Science, 2004 - science.org
L Yu, A Alva, H Su, P Dutt, E Freundt, S Welsh, EH Baehrecke, MJ Lenardo
Science, 2004science.org
Caspases play a central role in apoptosis, a well-studied pathway of programmed cell death.
Other programs of death potentially involving necrosis and autophagy may exist, but their
relation to apoptosis and mechanisms of regulation remains unclear. We define a new
molecular pathway in which activation of the receptor-interacting protein (a serine-threonine
kinase) and Jun amino-terminal kinase induced cell death with the morphology of
autophagy. Autophagic death required the genes ATG7 and beclin 1 and was induced by …
Caspases play a central role in apoptosis, a well-studied pathway of programmed cell death. Other programs of death potentially involving necrosis and autophagy may exist, but their relation to apoptosis and mechanisms of regulation remains unclear. We define a new molecular pathway in which activation of the receptor-interacting protein (a serine-threonine kinase) and Jun amino-terminal kinase induced cell death with the morphology of autophagy. Autophagic death required the genes ATG7 and beclin 1 and was induced by caspase-8 inhibition. Clinical therapies involving caspase inhibitors may arrest apoptosis but also have the unanticipated effect of promoting autophagic cell death.
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