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The activating transcription factor 2: an influencer of cancer progression

MUTAGENESIS (2019)

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Journal

MUTAGENESIS
Volume 34, Issue 5-6, Pages 375-389

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/mutage/gez041

Keywords

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Categories

Genetics & Heredity Toxicology

Funding

  1. European Cooperation in Science and Technology (COST) [CA17118]
  2. Bavarian-Czech University Agency [BTHA-JC-2019-1]
  3. Manfred-Stolte-Stiftung (Bayreuth, Germany)
  4. grant for the realization of equal opportunities for women in research and teaching by Bavarian state loans for the promotion of equality
  5. German Academic Exchange Service
  6. Academy of Sciences of the Czech Republic [RVO 68378050]
  7. Czech Centre for Phenogenomics by the Ministry of Education, Youth and Sports [LM2015040]
  8. Upgrade of the Czech Centre for Phenogenomics: developing towards translation research by the Ministry of Education, Youth and Sports and Education Research and Development Foundation [CZ.02.1.01/0.0/0.0/16_013/0 001789]
  9. Biotechnology and Biomedicine Centre of the Academy of Sciences [Z.1.05/1.1.00/02.0109]
  10. Higher quality and capacity for transgenic models by Ministry of Education, Youth and Sports and Education Research and Development Foundation [CZ.1.05/2.1.00/19.0395]
  11. Charles University in Vestec [Z.1.05/1.1.00/02.0109]

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In contrast to the continuous increase in survival rates for many cancer entities, colorectal cancer (CRC) and pancreatic cancer are predicted to be ranked among the top 3 cancer-related deaths in the European Union by 2025. Especially, fighting metastasis still constitutes an obstacle to be overcome in CRC and pancreatic cancer. As described by Fearon and Vogelstein, the development of CRC is based on sequential mutations leading to the activation of proto-oncogenes and the inactivation of tumour suppressor genes. In pancreatic cancer, genetic alterations also attribute to tumour development and progression. Recent findings have identified new potentially important transcription factors in CRC, among those the activating transcription factor 2 (ATF2). ATF2 is a basic leucine zipper protein and is involved in physiological and developmental processes, as well as in tumorigenesis. The mutation burden of ATF2 in CRC and pancreatic cancer is rather negligible; however, previous studies in other tumours indicated that ATF2 expression level and subcellular localisation impact tumour progression and patient prognosis. In a tissue- and stimulus-dependent manner, ATF2 is activated by upstream kinases, dimerises and induces target gene expression. Dependent on its dimerisation partner, ATF2 homodimers or heterodimers bind to cAMP-response elements or activator protein 1 consensus motifs. Pioneering work has been performed in melanoma in which the dual role of ATF2 is best understood. Even though there is increasing interest in ATF2 recently, only little is known about its involvement in CRC and pancreatic cancer. In this review, we summarise the current understanding of the underestimated 'cancer gene chameleon' ATF2 in apoptosis, epithelial-to-mesenchymal transition and microRNA regulation and highlight its functions in CRC and pancreatic cancer. We further provide a novel ATF2 3D structure with key phosphorylation sites and an updated overview of all so-far available mouse models to study ATF2 in vivo.

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