Attenuation of PTEN increases p21 stability and cytosolic localization in kidney cancer cells: a potential mechanism of apoptosis resistance

doi:10.1186/1476-4598-6-16

Molecular Cancer

Volume 6

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Lin PY
Fosmire SP
Park SH
Park JY
Baksh S
Modiano JF
Weiss RH

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Attenuation of PTEN increases p21 stability and cytosolic localization in kidney cancer cells: a potential mechanism of apoptosis resistance

Pei-Yin Lin¹ , Susan P Fosmire² , See-Hyoung Park¹ , Jin-Young Park¹ , Shairaz Baksh³ , Jaime F Modiano²^,4^* and Robert H Weiss¹^,5^*

¹Division of Nephrology, Department of Internal Medicine, University of California, Davis, CA, USA

²Integrated Department of Immunology, University of Colorado at Denver and Health Sciences Center, Denver, CO, USA

³Department of Pediatrics, University of Alberta, Edmonton, T6G 2H7, AB, Canada,

⁴University of Colorado Cancer Center, Aurora, CO, USA

⁵Department of Veterans' Affairs Northern California Health Care System, Sacramento, CA, USA

author email corresponding author email* Contributed equally

Molecular Cancer 2007, 6:16doi:10.1186/1476-4598-6-16


Published:	14 February 2007

Abstract

Background

The PTEN (Phosphatase and Tensin homolog deleted on chromosome Ten) tumor suppressor gene is frequently mutated or deleted in a wide variety of solid tumors, and these cancers are generally more aggressive and difficult to treat than those possessing wild type PTEN. While PTEN lies upstream of the phosphoinositide-3 kinase signaling pathway, the mechanisms that mediate its effects on tumor survival remain incompletely understood. Renal cell carcinoma (RCC) is associated with frequent treatment failures (~90% in metastatic cases), and these tumors frequently contain PTEN abnormalities.

Results

Using the ACHN cell line containing wild type PTEN, we generated a stable PTEN knockdown RCC cell line using RNA interference. We then used this PTEN knockdown cell line to show that PTEN attenuation increases resistance to cisplatin-induced apoptosis, a finding associated with increased levels of the cyclin kinase inhibitor p21. Elevated levels of p21 result from stabilization of the protein, and they are dependent on the activities of phosphoinositide-3 kinase and Akt. More specifically, the accumulation of p21 occurs preferentially in the cytosolic compartment, which likely contributes to both cell cycle progression and resistance to apoptosis.

Conclusion

Since p21 regulates a decision point between repair and apoptosis after DNA damage, our data suggest that p21 plays a key role in mechanisms used by PTEN-deficient tumors to escape chemotherapy. This in turn raises the possibility to use p21 attenuators as chemotherapy sensitizers, an area under active continuing investigation in our laboratories.