| Literature DB >> 24440709 |
Anke Rauch1, Dorle Hennig1, Claudia Schäfer1, Matthias Wirth2, Christian Marx1, Thorsten Heinzel1, Günter Schneider2, Oliver H Krämer3.
Abstract
Survivin belongs to the family of apoptosis inhibitors (IAPs), which antagonizes the induction of cell death. Dysregulated expression of IAPs is frequently observed in cancers, and the high levels of survivin in tumors compared to normal adult tissues make it an attractive target for pharmacological interventions. The small imidazolium-based compound YM155 has recently been reported to block the expression of survivin via inhibition of the survivin promoter. Recent data, however, question that this is the sole and main effect of this drug, which is already being tested in ongoing clinical studies. Here, we critically review the current data on YM155 and other new experimental agents supposed to antagonize survivin. We summarize how cells from various tumor entities and with differential expression of the tumor suppressor p53 respond to this agent in vitro and as murine xenografts. Additionally, we recapitulate clinical trials conducted with YM155. Our article further considers the potency of YM155 in combination with other anti-cancer agents and epigenetic modulators. We also assess state-of-the-art data on the sometimes very promiscuous molecular mechanisms affected by YM155 in cancer cells.Entities:
Keywords: Cancer; Chemotherapy; Molecular target; Specificity; Survivin; YM155
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Year: 2014 PMID: 24440709 DOI: 10.1016/j.bbcan.2014.01.003
Source DB: PubMed Journal: Biochim Biophys Acta ISSN: 0006-3002