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Literature DB >> 18381074

Small mitochondrial ARF (smARF) is located in both the nucleus and cytoplasm, induces cell death, and activates p53 in mouse fibroblasts.

Yuko Ueda¹, Terutsugu Koya, Noriko Yoneda-Kato, Jun-Ya Kato.

Abstract

The ARF transcript produces two proteins, the full-length ARF, p19(ARF), and a short mitochondrial version, smARF. To explore the functional difference between the two, we generated GFP-fused expression vectors for each protein and introduced them into NIH3T3 murine fibroblasts, which sustains a global deletion in the INK4a locus but contains a functional p53 gene. GFP-p19ARF was located within the nucleolus as previously reported, whereas GFP-smARF was detected mainly in the nucleoplasm. GFP-smARF induced cell death although to a slightly lesser extent than p19ARF. GFP-smARF stabilized p53 thereby inducing expression of the target genes, MDM2 and p21. We suggest that smARF has functions other than mitochondria-mediated autophagy, and induces p53 expression and cell death via a novel mechanism.

Entities: Disease Gene Species

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Year: 2008 PMID： 18381074 DOI： 10.1016/j.febslet.2008.03.032

Source DB: PubMed Journal: FEBS Lett ISSN： 0014-5793 Impact factor: 4.124

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Cited

7 in total

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Authors: Joshua L Justice; Brandy Verhalen; Ranjit Kumar; Elliot J Lefkowitz; Michael J Imperiale; Mengxi Jiang
Journal: J Proteome Res Date: 2015-09-23 Impact factor: 4.466

2. The ARF tumor suppressor can promote the progression of some tumors.

Authors: Olivier Humbey; Julia Pimkina; Jack T Zilfou; Michal Jarnik; Carmen Dominguez-Brauer; Darren J Burgess; Christine M Eischen; Maureen E Murphy
Journal: Cancer Res Date: 2008-12-01 Impact factor: 12.701

Review 3. p53 and ARF: unexpected players in autophagy.

Authors: Gregor M Balaburski; Robert D Hontz; Maureen E Murphy
Journal: Trends Cell Biol Date: 2010-03-19 Impact factor: 20.808

4. CDK inhibitors (p16/p19/p21) induce senescence and autophagy in cancer-associated fibroblasts, "fueling" tumor growth via paracrine interactions, without an increase in neo-angiogenesis.

Authors: Claudia Capparelli; Barbara Chiavarina; Diana Whitaker-Menezes; Timothy G Pestell; Richard G Pestell; James Hulit; Sebastiano Andò; Anthony Howell; Ubaldo E Martinez-Outschoorn; Federica Sotgia; Michael P Lisanti
Journal: Cell Cycle Date: 2012-08-30 Impact factor: 4.534

Small mitochondrial ARF (smARF) is located in both the nucleus and cytoplasm, induces cell death, and activates p53 in mouse fibroblasts.

1. Quantitative Proteomic Analysis of Enriched Nuclear Fractions from BK Polyomavirus-Infected Primary Renal Proximal Tubule Epithelial Cells.

2. The ARF tumor suppressor can promote the progression of some tumors.

Review 3. p53 and ARF: unexpected players in autophagy.

4. CDK inhibitors (p16/p19/p21) induce senescence and autophagy in cancer-associated fibroblasts, "fueling" tumor growth via paracrine interactions, without an increase in neo-angiogenesis.

Review 5. p53-Mediated Molecular Control of Autophagy in Tumor Cells.

Review 6. p53 Modulation of Autophagy Signaling in Cancer Therapies: Perspectives Mechanism and Therapeutic Targets.

7. Disruption of chromosome 11 in canine fibrosarcomas highlights an unusual variability of CDKN2B in dogs.