| Literature DB >> 22743622 |
O Merkel1, N Wacht, E Sifft, T Melchardt, F Hamacher, T Kocher, U Denk, J P Hofbauer, A Egle, M Scheideler, M Schlederer, M Steurer, L Kenner, R Greil.
Abstract
Chronic lymphocytic leukemia (CLL) is the most prevalent lymphoid malignancy in the elderly of the Western world. Although treatment options have improved over the past two decades, 10-15% of patients still have a poor prognosis and are often resistant to therapy. Aberrations in the p53 pathway, such as a deleted (del17p13) or mutated p53 gene, are highly enriched in this class of patients. In an extensive screen for p53-independent apoptosis inducers, actinomycin D was identified from 1496 substances and shown to induce apoptosis in primary CLL cells derived from high-risk patients including those with aberrant p53, revealing a novel p53-independent mechanism of action. Both pro-survival genes BCL2 and MCL1 are targeted by actinomycin D, in contrast to fludarabine the backbone of current treatment schedules. In the well-established TCL1 transgenic mouse model for high-risk CLL, actinomycin D treatment was more effective in reducing tumor load than fludarabine, with no evidence of resistance after three treatment cycles and an overall survival increase of over 300%. Tumor load reduction was coupled to BCL2 downregulation. Our results identify the clinically approved compound actinomycin D as a potentially valuable treatment option for CLL high-risk patients.Entities:
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Year: 2012 PMID: 22743622 DOI: 10.1038/leu.2012.147
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 11.528