Induction of autophagy and inhibition of tumorigenesis by beclin 1 (original) (raw)

• Letter
• Published: 09 December 1999
• Saadiya Jackson1,
• Matthew Seaman4,
• Kristy Brown2,3,
• Bettina Kempkes5,
• Hanina Hibshoosh2,3 &
• …
• Beth Levine1

Nature volume 402, pages 672–676 (1999)Cite this article

• 17k Accesses
• 2799 Citations
• 36 Altmetric
• Metrics details

Abstract

The process of autophagy, or bulk degradation of cellular proteins through an autophagosomic-lysosomal pathway1, is important in normal growth control and may be defective in tumour cells2. However, little is known about the genetic mediators of autophagy in mammalian cells or their role in tumour development. The mammalian gene encoding Beclin 1 (ref. 3), a novel Bcl-2-interacting, coiled-coil protein, has structural similarity to the yeast autophagy gene, apg6/vps30 (refs 4, 5), and is mono-allelically deleted in 40–75% of sporadic human breast cancers and ovarian cancers6. Here we show, using gene-transfer techniques, that beclin 1 promotes autophagy in autophagy-defective yeast with a targeted disruption of agp6/vps30, and in human MCF7 breast carcinoma cells. The autophagy-promoting activity of beclin 1 in MCF7 cells is associated with inhibition of MCF7 cellular proliferation, in vitro clonigenicity and tumorigenesis in nude mice. Furthermore, endogenous Beclin 1 protein expression is frequently low in human breast epithelial carcinoma cell lines and tissue, but is expressed ubiquitously at high levels in normal breast epithelia. Thus, beclin 1 is a mammalian autophagy gene that can inhibit tumorigenesis and is expressed at decreased levels in human breast carcinoma. These findings suggest that decreased expression of autophagy proteins may contribute to the development or progression of breast and other human malignancies.

This is a preview of subscription content, access via your institution

Access options

Subscribe to this journal

Receive 51 print issues and online access

$199.00 per year

only $3.90 per issue

Buy this article

• Purchase on SpringerLink
• Instant access to full article PDF

Prices may be subject to local taxes which are calculated during checkout

Additional access options:

• Log in
• Learn about institutional subscriptions
• Read our FAQs
• Contact customer support

Similar content being viewed by others

References

1. Dunn,W. A. J. Autophagy and related mechanisms of lyosomal-mediated protein degradation. Trends Cell Biol. 4, 139– 143 (1994).
   Article CAS Google Scholar
2. Kisen,G. O. et al. Reduced autophagic activity in primary rat hepatocellular carcinoma and ascites hepatoma cells. Carcinogenesis 14, 2501–2505 (1993).
   Article CAS Google Scholar
3. Liang,X. H. et al. Protection against fatal Sindbis virus encephalitis by Beclin, a novel Bcl-2-interacting protein. J. Virol. 72, 8586–8596 (1998).
   CAS PubMed PubMed Central Google Scholar
4. Kametaka,S., Okano,T., Ohsumi,M. & Ohsumi,Y. Apg14p and Apg6/Vps30p form a protein complex essential for autophagy in the yeast, Saccharomyces cerevisiae. J. Biol. Chem. 273, 22284 –22291 (1998).
   Article CAS Google Scholar
5. Seaman,M. N. J., Marcusson,E. G., Cereghino, J. L. & Emr,S. D. Endosome to golgi retrieval of the vacuolar protein sorting receptor, Vps10p, requires the function of the VPS29, VPS30, and VPS35 gene products. J. Cell. Biol. 137, 79–92 (1997).
   Article CAS Google Scholar
6. Aita,V. M. et al. Cloning and genomic structure of beclin 1, a candidate tumor suppressor gene on chromosome 17q21. Genomics 59, 59–65 (1999).
   Article CAS Google Scholar
7. Tsukada,M. & Ohsumi,Y. Isolation and characterization of autophagy-defective mutants of Saccharomyces cerevisiae. FEBS 333, 169–174 (1993).
   Article CAS Google Scholar
8. Kametaka,S., Matsuura,A., Wada,Y. & Ohsumi,Y. Structural and functional analyses of APG5, a gene involved in autophagy in yeast. Gene 178, 139–143 (1996).
   Article CAS Google Scholar
9. Friedman,L. S. et al. The search for BRCA1. Cancer Res. 54 , 6374–6382 (1994).
   CAS PubMed Google Scholar
10. Rommens,J. M. et al. Generation of a transcription map at the HSD17B locus centromeric to BRCA1 at 17q21. Genomics 28, 530– 542 (1995).
    Article CAS Google Scholar
11. Holt,J. T. et al. Growth retardation and tumour inhibition by BRCA1. Nature Genet. 12, 298–302 (1996).
    Article CAS Google Scholar
12. Wu,K.-J., Polack,A. & Dalla-Favera, R. Coordinated regulation of iron-controlling genes, H-ferritin and IRP2, by c-MYC. Science 283, 676– 679 (1999).
    Article ADS CAS Google Scholar
13. Mortimore,G. E. & Poso,A. R. Amino acid control of intracellular protein degradation. Methods Enzymol. 166, 461–476 (1988).
    Article CAS Google Scholar
14. Dunn,W. A. Studies on the mechanisms of autophagy; formation of the autophagic vacuole. J. Cell. Biol. 110, 1923– 1933 (1990).
    Article Google Scholar
15. Dunn,W. A. Studies on the mechanisms of autophagy; maturation of the autophagic vacuole. J. Cell. Biol. 110, 1935– 1945 (1990).
    Article CAS Google Scholar
16. Mitchener,J. S., Shelburne,J. D., Bradford, W. D. & Hawkins,H. K. Cellular autophagocytosis induced by deprivation of serum and amino acids in HeLa cells. Am. J. Pathol. 83, 485– 498 (1976).
    CAS PubMed PubMed Central Google Scholar
17. Seglen,P. O. & Gordon,P. B. 3-methyladenine: specific inhibitor of autophagic/lysosomal protein degradation in isolated rat hepatocytes. Proc. Natl Acad. Sci. USA 79, 1889– 1892 (1982).
    Article ADS CAS Google Scholar
18. Bradley,M. O. Regulation of protein degradation in normal and transformed human cells. J. Biol. Chem. 252, 5310–5315 (1977).
    CAS PubMed Google Scholar
19. Lee,H.-K., Jones,R. T., Myers,R. A. M. & Marzella,L. Regulation of protein degradation in normal and transformed human bronchial epithelial cells in culture. Arch. Biochem. Biophys. 296, 271–278 (1992).
    Article CAS Google Scholar
20. Gunn,J. M., Clark,M. G., Knowles,S. E., Hopgood,M. F. & Ballard,F. J. Reduced rates of proteolysis in transformed cells. Nature 266, 58– 60 (1977).
    Article ADS CAS Google Scholar
21. Gronostajski,R. M. & Pardee,A. B. Protein degradation in 3T3 and tumorigenic transformed 3T3 cells. J. Cell. Physiol. 119, 127–132 (1984).
    Article CAS Google Scholar
22. Knecht,E., Hernandez-Yago,J. & Grisolia, S. Regulation of lysosomal autophagy in transformed and non-transformed mouse fibroblasts under several growth conditions. Exp. Cell. Res. 154, 224–232 (1984).
    Article CAS Google Scholar
23. Otsuka,H. & Moskowitz,M. Differences in the rates of protein degradation in untransformed and transformed cell lines. Exp. Cell. Res. 112, 127–135 (1978).
    Article CAS Google Scholar
24. Blommaart,E. F. C., Luiken,J. J. F. P., Blommaart, P. J. E., vanWoerkom,G. M. & Meijer,A. J. Phosphorylation of ribosomal protein S6 is inhibitory for autophagy in isolated rat hepatocytes. J. Biol. Chem. 270, 2320– 2326 (1995).
    Article CAS Google Scholar
25. Eble,R. A simple and efficient procedure for transformation of yeasts. Biotechniques 13, 18–20 (1992).
    Google Scholar
26. Oldenburg,K. R., Vo,K. T., Michaelis,S. & Paddon,C. Recombination-mediated PCR-directed plasmid construction in vivo in yeast. Nucleic Acids Res. 25, 451–452 (1997).
    Article CAS Google Scholar
27. Jiang,W. & Al,E. Overexpression of cyclin D1 in rat fibroblasts causes abnormalities in growth control, cell cycle progression and gene expression. Oncogene 8, 3447–3457 (1993).
    CAS PubMed Google Scholar

Download references

Acknowledgements

We thank R. Rothstein and L. Pons for helpful discussions, and J. Kitajewski and R. Dalla-Favera for providing reagents. This work was supported by the NIH, the American Cancer Society, an Irma T. Hirschl Trust Award and an Elaine B. Lesser Award in Ovarian Cancer Research.

Author information

Authors and Affiliations

1. Department of Medicine,
   Xiao Huan Liang, Saadiya Jackson & Beth Levine
2. Department of Pathology, Columbia University College of Physicians & Surgeons, New York, 10032, New York, USA
   Kristy Brown & Hanina Hibshoosh
3. Surgeons,
   Kristy Brown & Hanina Hibshoosh
4. Department of Clinical Biochemistry Cambridge Institute for Medical Research, Addenbrookes Hospital, Cambridge, CB2 2XY, UK
   Matthew Seaman
5. Institute for Clinical Molecular Biology, GSF-National Research Center for Environment and Health, Munich, 81377, Germany
   Bettina Kempkes

Authors

1. Xiao Huan Liang
   You can also search for this author inPubMed Google Scholar
2. Saadiya Jackson
   You can also search for this author inPubMed Google Scholar
3. Matthew Seaman
   You can also search for this author inPubMed Google Scholar
4. Kristy Brown
   You can also search for this author inPubMed Google Scholar
5. Bettina Kempkes
   You can also search for this author inPubMed Google Scholar
6. Hanina Hibshoosh
   You can also search for this author inPubMed Google Scholar
7. Beth Levine
   You can also search for this author inPubMed Google Scholar

Corresponding author

Correspondence toBeth Levine.

Rights and permissions

About this article

Cite this article

Liang, X., Jackson, S., Seaman, M. et al. Induction of autophagy and inhibition of tumorigenesis by beclin 1 .Nature 402, 672–676 (1999). https://doi.org/10.1038/45257

Download citation

• Received: 03 June 1999
• Accepted: 29 September 1999
• Issue Date: 09 December 1999
• DOI: https://doi.org/10.1038/45257

This article is cited by