252979-56-9
| 中文名称 | 252979-56-9 |
|---|---|
| 中文同义词 | 1,4-双[[2-(二甲氧基氨基氨基)乙基]氨基] -5,8-二羟基-9,10-蒽二酮;巴诺蒽醌 二盐酸盐;化合物 T10459;巴诺蒽醌盐酸盐;2,2'-((5,8-二羟基-9,10-二氧代-9,10-二氢蒽-1,4-二基)双(氮杂二基))双(N,N-二甲基乙胺氧化物)二盐酸盐;BANOXANTRONE DIHYDROCHLORIDE (AQ4N),TOPOISOMERASE II抑制剂;巴诺蒽醌盐酸盐,10 MM DMSO 溶液 |
| 英文名称 | Banoxantrone (dihydrochloride) |
| 英文同义词 | Banoxantrone 2HCl;1,4-Bis[[2-(dimethyloxidoamino)ethyl]amino]-5,8-dihydroxy-9,10-anthracenedione dihydrochloride;AQ4N dihydrochloride;Banoxantrone dihydrochloride >=98% (HPLC);2,2'-((5,8-Dihydroxy-9,10-dioxo-9,10-dihydroanthracene-1,4-diyl)bis(azanediyl))bis(N,N-dimethylethanamine oxide) dihydrochloride , Banoxantrone 2HCl;2,2'-((5,8-Dihydroxy-9,10-dioxo-9,10-dihydroanthracene-1,4-diyl)bis(azanediyl))bis(N,N-dimethylethanamine oxide) dihydrochloride;Banoxantrone dihydrochloride (AQ4N), Topoisomerase II inhibitor;Banoxantrone dihydrochloride, 10 mM in DMSO |
| CAS号 | 252979-56-9 |
| 分子式 | C22H29ClN4O6 |
| 分子量 | 480.95 |
| EINECS号 | |
| 相关类别 | |
| Mol文件 | 252979-56-9.mol |
| 结构式 |  |
252979-56-9 性质
| 储存条件 | Store at -20°C, protect from light, stored under nitrogen |
|---|---|
| 溶解度 | 在水中溶解度为 50 mM,在 DMSO 中溶解度为 25 mM |
| 形态 | 固体 |
| 颜色 | 蓝至深蓝 |
| 水溶解性 | Water : 25 mg/mL (48.32 mM) |
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Topoisomerase II
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Banoxantrone (AQ4N) can be reduced in a hypoxic environment to a stable DNA-affinic agent AQ4. AQ4, a potent topoisomerase II inhibitor, would be capable of damaging cells recruited into the cell cycle following radiation damage to the well-oxygenated cells of the tumor. Banoxantrone shows more than 8-fold higher cytotoxicity under hypoxia than normoxia in cultures of 9L rat gliosarcoma and H460 human non-small-cell lung carcinoma cells but not for 11 other human cancer cell lines. DT-diaphorase protein levels and banoxantrone chemosensitivity are poorly correlated across the cancer cell line panel, and banoxantrone chemosensitivity is not affected by DT-diaphorase inhibitors. Banoxantrone is a bis-N-oxide that is reduced via two sequential two-electron reductions to the tertiary amine, AQ4, which is a potent cytotoxic agent toward both aerobic and hypoxic cells. AQ4, but not AQ4N, intercalates in DNA with high affinity to generate a stable persistent complex that can inhibit topoisomerase II and cause DNA damage and cell death.
Banoxantrone (200 mg/kg) significantly enhances the tumor growth delay caused by radiation. This occurred when radiation is administered both as a single dose (12 Gy) and in a multifraction regimen (5x3 Gy). A study of the scheduling of Banoxantrone (AQ4N) administration shows that there is a very long time period over which a maximal effect can be elicited (drug given 4 days before to 6 h after radiation). These results suggest that Banoxantrone has significant potential as a bioreductive drug. The activation of banoxantrone cytotoxicity in vivo requires tumor hypoxia that is more extensive or prolonged than can readily be achieved by vasodilation or by antiangiogenic drug treatment. Incorporation of banoxantrone into conventional chemoradiation protocols therefore targets both oxygenated and hypoxic regions of tumors, and potentially will increase the effectiveness of therapy. A single dose of 60 mg/kg banoxantrone enhances the response of RT112 (bladder) and Calu-6 (lung) xenografts to treatment with cisplatin and radiation therapy. Banoxantrone will increase the efficacy of chemoradiotherapy in preclinical models.