Preclinical anti‐myeloma activity of the novel HDAC‐inhibitor JNJ‐26481585 |
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Authors: | Thorsten Stühmer Janine Arts Manik Chatterjee Johanna Borawski André Wolff Peter King Hermann Einsele Eugen Leo Ralf C. Bargou |
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Affiliation: | 1. Department of Internal Medicine II, Division of Haematology, University Hospital of Würzburg, Würzburg, Germany;2. Ortho Biotech Oncology Research and Development, Beerse, Belgium |
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Abstract: | Pharmacological inhibitors of histone deacetylases (HDACs) are currently being developed and tested as anti‐cancer agents and may be useful to enhance the therapeutic efficiency of established anti‐myeloma treatments. This study preclinically evaluated the effects of the ‘second generation’ pan‐HDAC inhibitor JNJ‐26481585 on human multiple myeloma (MM) cells from established cell lines and primary MM samples (n = 42). Molecular responses in both groups of MM cells included histone acetylation, a shift in Bcl2‐family members towards proapoptotic bias, attenuation of growth and survival pathway activity and Hsp72 induction. Mcl‐1 depletion and Hsp72 induction were the most reliable features observed in JNJ‐26481585‐treated primary MM samples. The drug alone effectively induced myeloma cell death at low nanomolar concentrations. In vitro combination of JNJ‐26481585 with anti‐myeloma therapeutic agents generally resulted In effects close to additivity. In view of the favourable activity of this novel HDAC‐inhibitor towards primary myeloma cells further evaluation in a clinical setting is warranted. |
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Keywords: | multiple myeloma histone deacetylase inhibitor novel agent |
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