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Mechanisms of Action of the Anti-cancer Organic Arsenical Darinaparsin: Cellular Import, Intracellular Signalling, Gene Expression and Potency of the Anti-cancer Organic Arsenical Darinaparsin Nicolas Garnier
Mechanisms of Action of the Anti-cancer Organic Arsenical Darinaparsin: Cellular Import, Intracellular Signalling, Gene Expression and Potency of the Anti-cancer Organic Arsenical Darinaparsin
Nicolas Garnier
Arsenic trioxide (ATO) is a successful treatment for Acute Promyelocytic Leukemia (APL), but other cancers remain mildly sensitive to ATO at clinically achievable doses. Moreover, APL cells can develop resistance to ATO. Darinaparsin (S-dimethylarsino-GSH; Dar) is a more potent apoptosis-inducing arsenical than ATO in various cancer models. It also has a maximum tolerated dose that is 35-fold higher than ATO. Dar accumulates in the cell to a greater extent that ATO, which led to hypothesize that Dar import might contribute to its enhanced efficacy. We found that Dar gets transformed extracellularly and imported via cystine/cysteine importing systems. We also hypothesized that the increased cytotoxicity of Dar may be due to a decreased cytoprotective response. We found that a lack of HO-1 activation is partially responsible for Dar?s enhanced anti-tumor properties. Cells respond to arsenicals by increasing cystine uptake and HO-1 expression, which leads to protection against ATO but hypersensitivity to Dar. This work encompasses many aspects of modern molecular pharmacology, experimental oncology, and should inspire future efforts towards designing arsenic-based anti-cancer drugs.
| Medios de comunicación | Libros Paperback Book (Libro con tapa blanda y lomo encolado) |
| Publicado | 28 de febrero de 2014 |
| ISBN13 | 9783659132728 |
| Editores | LAP LAMBERT Academic Publishing |
| Páginas | 120 |
| Dimensiones | 150 × 7 × 225 mm · 197 g |
| Lengua | Alemán |
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