Abstract

The notorious resistance of melanoma cells to radiation and chemotherapy has been a major obstacle to the treatment of tumors of this type. Studies performed in our laboratory over the past few years identified ATF2 as an important contributor to melanoma's resistance to radiation and chemical treatment. Our studies revealed that ATF2 is capable of altering death-signaling cascades in human melanoma cells. Accordingly, we sought to determine whether interfering with endogenous ATF2 transcriptional activities would alter the resistance of melanoma cells to radiation and chemotherapy. Forced expression of a peptide corresponding to amino acids 50-100 of ATF2 (ATF250-100) resulted in reduced resistance of late stage melanoma cells to radiation as well as to a series of chemotherapeutic agents. Such sensitization was enhanced when the expression of the ATF2 peptide was combined with the pharmacological inhibitor of stress kinases. Injection of ATF250-100 expressing human melanoma cells into nude mice led to an efficient decrease in tumor growth upon treatment with chemotherapeutic drugs or the pharmacological inhibitor of p38 MAPK. Forced expression in mouse melanoma models SW1 or B16F10 resulted in significant inhibition of tumor growth--to the point of complete regression and inhibition of metastasis depending on the mode of peptide administration. These findings point to the possible use of the ATF2 peptide for reducing melanoma tumorigenicity and metastasis. Mechanisms underlying the effect of the ATF2 peptide were shown to include decreased ATF2 and increased c-Jun transcriptional activities, which result in sensitization to apoptosis. Here we propose to extend these observations towards better assessment of the mechanisms underlying the effect of the ATF2 peptide and further explore, in the in vivo setting, ways to improve the ATF2 peptide's effect. To this end we propose to: (I) Identify the changes in ATF2 and c-Jun function and activities in the course of melanoma development and progression (gene mutation, RNA and protein expression and phosphorylation); (II) Determine the primary mechanism underlying the changes in ATF2 and c-Jun expression and activities in tumors that express the ATF2 peptide. (III) Assess whether a modified ATF2 peptide, either by mutations and truncations that affect phosphoacceptor sites or conformationally important domains, would elicit the biological changes in melanoma, in vitro and in vivo, that are seen with the 50 aa peptide; (IV) Assess the role of the immune response against the ATF2 peptide's expressing melanomas in vivo. Determine whether the ATF2 peptide expression in tumors elicits greater effects in vivo when combined with different treatments, including immune modulators and IL-12. (V) Identify the profile of genes that are commonly induced or suppressed in ATF2 peptide-expressing tumors on the basis of analysis of three tumor types in three mouse strains.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
7R01CA099961-03
Application #
6891665
Study Section
Chemical Pathology Study Section (CPA)
Program Officer
Jhappan, Chamelli
Project Start
2003-05-01
Project End
2008-04-30
Budget Start
2005-05-01
Budget End
2006-04-30
Support Year
3
Fiscal Year
2005
Total Cost
$424,975
Indirect Cost

  Institution

Name
Sanford-Burnham Medical Research Institute
Department
Type
DUNS #
020520466
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Claps, Giuseppina; Cheli, Yann; Zhang, Tongwu et al. (2016) A Transcriptionally Inactive ATF2 Variant Drives Melanomagenesis. Cell Rep 15:1884-92
Scortegagna, Marzia; Kim, Hyungsoo; Li, Jian-Liang et al. (2014) Fine tuning of the UPR by the ubiquitin ligases Siah1/2. PLoS Genet 10:e1004348
Scortegagna, M; Ruller, C; Feng, Y et al. (2014) Genetic inactivation or pharmacological inhibition of Pdk1 delays development and inhibits metastasis of Braf(V600E)::Pten(-/-) melanoma. Oncogene 33:4330-9
Varsano, Tal; Lau, Eric; Feng, Yongmei et al. (2013) Inhibition of melanoma growth by small molecules that promote the mitochondrial localization of ATF2. Clin Cancer Res 19:2710-22
Qi, Jianfei; Kim, Hyungsoo; Scortegagna, Marzia et al. (2013) Regulators and effectors of Siah ubiquitin ligases. Cell Biochem Biophys 67:15-24
Feng, Yongmei; Lau, Eric; Scortegagna, Marzia et al. (2013) Inhibition of melanoma development in the Nras((Q61K)) ::Ink4a(-/-) mouse model by the small molecule BI-69A11. Pigment Cell Melanoma Res 26:136-42
Lau, Eric; Ronai, Ze'ev A (2012) ATF2 - at the crossroad of nuclear and cytosolic functions. J Cell Sci 125:2815-24
Lau, Eric; Kluger, Harriet; Varsano, Tal et al. (2012) PKC? promotes oncogenic functions of ATF2 in the nucleus while blocking its apoptotic function at mitochondria. Cell 148:543-55
Shah, Meera; Bhoumik, Anindita; Goel, Vikas et al. (2010) A role for ATF2 in regulating MITF and melanoma development. PLoS Genet 6:e1001258
Lopez-Bergami, Pablo; Lau, Eric; Ronai, Ze'ev (2010) Emerging roles of ATF2 and the dynamic AP1 network in cancer. Nat Rev Cancer 10:65-76

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