Valproic acid exerts anti-tumor as well as anti-angiogenic effects on myeloma

Multiple myeloma is still an incurable disease, most commonly occurring in the elderly. The myeloma-induced bone marrow microenvironment protects myeloma cells from drug-induced apoptosis. Therefore, the development of novel and tolerable therapeutic alternatives to overcome the drug resistance is a...

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Veröffentlicht in:International journal of hematology 2009-01, Vol.89 (1), p.45-57
Hauptverfasser: Kitazoe, Ken-ichi, Abe, Masahiro, Hiasa, Masahiro, Oda, Asuka, Amou, Hiroe, Harada, Takeshi, Nakano, Ayako, Takeuchi, Kyoko, Hashimoto, Toshihiro, Ozaki, Shuji, Matsumoto, Toshio
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Sprache:eng
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Zusammenfassung:Multiple myeloma is still an incurable disease, most commonly occurring in the elderly. The myeloma-induced bone marrow microenvironment protects myeloma cells from drug-induced apoptosis. Therefore, the development of novel and tolerable therapeutic alternatives to overcome the drug resistance is an important clinical issue. Valproic acid (VPA), a safe and widely used anti-epileptic agent, is revisited as a class I- and IIa-specific histone deacetylase inhibitor. In the present study, we evaluated the effect as well as a mechanism of actions of VPA on myeloma cell growth and survival, with special reference to the myeloma-induced bone marrow microenvironment. VPA at therapeutic concentrations for epilepsy induced cell death in primary CD138-positive myeloma cells as well as myeloma cell lines, but not in CD138-negative bone marrow cells. VPA suppressed osteoclastogenesis as well as osteoclast-mediated myeloma cell growth. VPA also inhibited vascular tubule formation enhanced by co-cultures of myeloma cells and osteoclasts in concert with thalidomide. In addition, VPA induced both caspase-dependent and -independent cell death in myeloma cells, and potentiated the anti-myeloma effects of melphalan and dexamethasone. Collectively, VPA is suggested to exert multi-factorial anti-myeloma actions, and may serve as a safe adjuvant to be included in conventional chemotherapies against myeloma.
ISSN:0925-5710
1865-3774
DOI:10.1007/s12185-008-0226-9