Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine

Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine

Dacarbazine (DTIC) has been used for the treatment of melanoma for decades. However, monotherapy with this chemotherapeutic agent results only in moderate response rates. To improve tumor response to DTIC current clinical trials in melanoma focus on combining a novel targeted agent with chemotherapy...

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Main Authors: Thilakavathy Thangasamy, Sivanandane Sittadjody, Kirsten H. Limesand, Randy Burd
Format: Article
Language:English
Published: Hindawi Limited 2008-01-01
Series:Cellular Oncology
Online Access:http://dx.doi.org/10.3233/CLO-2008-0441
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spelling doaj-cd6144c9c78741e78e1b53a16a215e2b2020-11-25T00:11:57ZengHindawi LimitedCellular Oncology1570-58701875-86062008-01-0130537138710.3233/CLO-2008-0441Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to DacarbazineThilakavathy Thangasamy0Sivanandane Sittadjody1Kirsten H. Limesand2Randy Burd3Department of Nutritional Sciences, University of Arizona, Tucson, AZ 85721, USADepartment of Nutritional Sciences, University of Arizona, Tucson, AZ 85721, USADepartment of Nutritional Sciences, University of Arizona, Tucson, AZ 85721, USADepartment of Nutritional Sciences, University of Arizona, Tucson, AZ 85721, USADacarbazine (DTIC) has been used for the treatment of melanoma for decades. However, monotherapy with this chemotherapeutic agent results only in moderate response rates. To improve tumor response to DTIC current clinical trials in melanoma focus on combining a novel targeted agent with chemotherapy. Here, we demonstrate that tyrosinase which is commonly overexpressed in melanoma activates the bioflavonoid quercetin (Qct) and promotes an ataxia telangiectasia mutated (ATM)-dependent DNA damage response. This response sensitizes melanoma cells that overexpress tyrosinase to DTIC. In DB-1 melanoma cells that overexpress tyrosinase (Tyr+ cells), the threshold for phosphorylation of ATM and p53 at serine 15 was observed at a low dose of Qct (25 μM) when compared to the mock transfected pcDNA3 cells, which required a higher dose (75 μM). Both pcDNA3 and Tyr+ DB-1 cells demonstrated similar increases in phosphorylation of p53 at other serine sites, but in the Tyr+ cells, DNApk expression was found to be reduced compared to control cells, indicating a shift towards an ATM-mediated response. The DB-1 control cells were resistant to DTIC, but were sensitized to apoptosis with high dose Qct, while Tyr+ cells were sensitized to DTIC with low or high dose Qct. Qct also sensitized SK Mel 5 (p53 wildtype) and 28 (p53 mutant) cells to DTIC. However, when SK Mel 5 cells were transiently transfected with tyrosinase and treated with Qct plus DTIC, SK Mel 5 cells demonstrated a more than additive induction of apoptosis. Therefore, this study demonstrates that tyrosinase overexpression promotes an ATM-dependent p53 phosphorylation by Qct treatment and sensitizes melanoma cells to dacarbazine. In conclusion, these results suggest that Qct or Qct analogues may significantly improve DTIC response rates in tumors that express tyrosinase.http://dx.doi.org/10.3233/CLO-2008-0441
collection DOAJ
language English
format Article
sources DOAJ
author Thilakavathy Thangasamy
Sivanandane Sittadjody
Kirsten H. Limesand
Randy Burd
spellingShingle Thilakavathy Thangasamy
Sivanandane Sittadjody
Kirsten H. Limesand
Randy Burd
Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine
Cellular Oncology
author_facet Thilakavathy Thangasamy
Sivanandane Sittadjody
Kirsten H. Limesand
Randy Burd
author_sort Thilakavathy Thangasamy
title Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine
title_short Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine
title_full Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine
title_fullStr Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine
title_full_unstemmed Tyrosinase Overexpression Promotes ATM-Dependent p53 Phosphorylation by Quercetin and Sensitizes Melanoma Cells to Dacarbazine
title_sort tyrosinase overexpression promotes atm-dependent p53 phosphorylation by quercetin and sensitizes melanoma cells to dacarbazine
publisher Hindawi Limited
series Cellular Oncology
issn 1570-5870
1875-8606
publishDate 2008-01-01
description Dacarbazine (DTIC) has been used for the treatment of melanoma for decades. However, monotherapy with this chemotherapeutic agent results only in moderate response rates. To improve tumor response to DTIC current clinical trials in melanoma focus on combining a novel targeted agent with chemotherapy. Here, we demonstrate that tyrosinase which is commonly overexpressed in melanoma activates the bioflavonoid quercetin (Qct) and promotes an ataxia telangiectasia mutated (ATM)-dependent DNA damage response. This response sensitizes melanoma cells that overexpress tyrosinase to DTIC. In DB-1 melanoma cells that overexpress tyrosinase (Tyr+ cells), the threshold for phosphorylation of ATM and p53 at serine 15 was observed at a low dose of Qct (25 μM) when compared to the mock transfected pcDNA3 cells, which required a higher dose (75 μM). Both pcDNA3 and Tyr+ DB-1 cells demonstrated similar increases in phosphorylation of p53 at other serine sites, but in the Tyr+ cells, DNApk expression was found to be reduced compared to control cells, indicating a shift towards an ATM-mediated response. The DB-1 control cells were resistant to DTIC, but were sensitized to apoptosis with high dose Qct, while Tyr+ cells were sensitized to DTIC with low or high dose Qct. Qct also sensitized SK Mel 5 (p53 wildtype) and 28 (p53 mutant) cells to DTIC. However, when SK Mel 5 cells were transiently transfected with tyrosinase and treated with Qct plus DTIC, SK Mel 5 cells demonstrated a more than additive induction of apoptosis. Therefore, this study demonstrates that tyrosinase overexpression promotes an ATM-dependent p53 phosphorylation by Qct treatment and sensitizes melanoma cells to dacarbazine. In conclusion, these results suggest that Qct or Qct analogues may significantly improve DTIC response rates in tumors that express tyrosinase.
url http://dx.doi.org/10.3233/CLO-2008-0441
work_keys_str_mv AT thilakavathythangasamy tyrosinaseoverexpressionpromotesatmdependentp53phosphorylationbyquercetinandsensitizesmelanomacellstodacarbazine
AT sivanandanesittadjody tyrosinaseoverexpressionpromotesatmdependentp53phosphorylationbyquercetinandsensitizesmelanomacellstodacarbazine
AT kirstenhlimesand tyrosinaseoverexpressionpromotesatmdependentp53phosphorylationbyquercetinandsensitizesmelanomacellstodacarbazine
AT randyburd tyrosinaseoverexpressionpromotesatmdependentp53phosphorylationbyquercetinandsensitizesmelanomacellstodacarbazine
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