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    Mol Cell. 2006 May 19;22(4):463-75.

    A short mitochondrial form of p19ARF induces autophagy and caspase-independent cell death.

    Reef S, Zalckvar E, Shifman O, Bialik S, Sabanay H, Oren M, Kimchi A.

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    Department of Molecular Genetics, Weizmann Institute of Science, Rehovot, Israel.

    Abstract

    The tumor suppressor functions of p19(ARF) have been attributed to its ability to induce cell cycle arrest or apoptosis by activating p53 and regulating ribosome biogenesis. Here we describe another cellular function of p19(ARF), involving a short isoform (smARF, short mitochondrial ARF) that localizes to a Proteinase K-resistant compartment of the mitochondria. smARF is a product of internal initiation of translation at Met45, which lacks the nucleolar functional domains. The human p14(ARF) mRNA likewise produces a shorter isoform. smARF is maintained at low levels via proteasome-mediated degradation, but it increases in response to viral and cellular oncogenes. Ectopic expression of smARF reduces mitochondrial membrane potential (DeltaPsim) without causing cytochrome c release or caspase activation. The dissipation of DeltaPsim does not depend on p53 or Bcl-2 family members. smARF induces massive autophagy and caspase-independent cell death that can be partially rescued by knocking down ATG5 or Beclin-1, suggesting a different prodeath function for this short isoform.

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    PMID:
    16713577
    [PubMed - indexed for MEDLINE]

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