AldoxorubicinCAS号1361644-26-9
AldoxorubicinCAS号1361644-26-9
AldoxorubicinCAS号1361644-26-9
AldoxorubicinCAS号1361644-26-9

Aldoxorubicin

¥545.00 ~¥1,730.00
10mg / 5mg / 2mg
10mg
北京
索莱宝
2026-04-10
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产品详情
中文名称:Aldoxorubicin中文别名:Aldoxorubicin
英文名称:AldoxorubicinCAS:1361644-26-9
产品分类:小分子化合物纯度:≥98%
产品编号品牌纯度规格库存价格
IA6520索莱宝≥98%10mg有现货1,730.00 元
IA6520索莱宝≥98%5mg有现货987.00 元
IA6520索莱宝≥98%2mg有现货545.00 元
标准名称:INNO-206英文名称:Aldoxorubicin
CAS:1361644-26-9分子式:C37H42N4O13
分子量:750.748390674591颜色与性状:
密度:1.60±0.1 g/cm3 (20 ºC 760 Torr),沸点:
熔点:水溶性:
CAS1361644-26-9
英文名称Aldoxorubicin
别名INNO-206;ALDOXORUBICIN;CS-1186;Aldoxorubicin(USAN);DOXO-EMCH;
分子式C37H42N4O13
分子量750.75
规格2mg ; 5mg ; 10mg
溶解性Soluble in DMSO ≥5mg/mL(Need ultrasonic)(该产品在溶液状态不稳定,建议您现用现配)
纯度≥98%
级别Cell Culture
外观(性状)Solid
储存条件Powder:-20℃,2 years
运输条件冷藏运输
MDLMFCD15146982
SMILESC[C@H]1[C@H]([C@H](C[C@@H](O1)O[C@H]2C[C@@](CC3=C2C(=C4C(=C3O)C(=O)C5=C(C4=O)C(=CC=C5)OC)O)(/C(=N/NC(=O)CCCCCN6C(=O)C=CC6=O)/CO)O)N)O
InChIKeyOBMJQRLIQQTJLR-USGQOSEYSA-N
InChIInChI=1S/C37H42N4O13/c1-17-32(46)20(38)13-27(53-17)54-22-15-37(51,23(16-42)39-40-24(43)9-4-3-5-12-41-25(44)10-11-26(41)45)14-19-29(22)36(50)31-30(34(19)48)33(47)18-7-6-8-21(52-2)28(18)35(31)49/h6-8,10-11,17,20,22,27,32,42,46,48,50-51H,3-5,9,12-16,38H2,1-2H3,(H,40,43)/b39-23+/t17-,20-,22-,27-,32+,37-/m0/s1
PubChem CID9810709
靶点Others
通路Others
背景说明是一种化合物,具有抗肿瘤活性。
生物活性Aldoxorubicin (INNO-206) is an albumin-binding proagent of Doxorubicin (DNA topoisomerase II inhibitor), which is released from albumin under acidic conditions. Aldoxorubicin (INNO-206) has potent antitumor activities in various cancer cell lines and in murine tumor models.[1-4]
In VitroAldoxorubicin (INNO-206)? (0.27 to 2.16 μM) inhibits blood vessel formation and reduces multiple myeloma cell growth in a pH-dependent fashion[1].
In VivoAldoxorubicin (INNO-206) (10.8 mg/kg, i.v.) shows significantly smaller tumor volumes and IgG levels on days 28, and is well tolerated with 90% of mice surviving until the termination of the study in the mice bearing the LAGκ-1A tumor[1]. Aldoxorubicin (INNO-206) shows a good safety profile at doses up to 260 mg/mL doxorubicin equivalents, and is able to induce tumor regressions in breast cancer, small cell lung cancer and sarcoma in phase I study[2]. Aldoxorubicin (INNO-206) shows superior activity over doxorubicin in a murine renal cell carcinoma model and in breast carcinoma xenograft models[3].
细胞实验Cells are seeded at 1×105?cells/100 μL/well in 96-well plates in RPMI-1640 media with FBS for 24 hours before treatment. Cells are cultured in the presence of medium, Aldoxorubicin (INNO-206) or doxorubicin for 48 hours. Next, cell viability is quantified using the CellTiter 96 AQueous Non-Radioactive Cell Proliferation Assay. Each well is treated with MTS for 1 to 4 hours, after which absorbance at 490 nm is recorded using a 96-well plate reader. The quantity of formazan product as measured is directly proportional to the number of living cells. Data graphed are means±SEM using 3 replicates per data point.[1-4]
动物实验For the LAGκ-1A experiment, Aldoxorubicin (INNO-206) is administered to SCID mice at 10.8 mg/kg (doxorubicin equivalent dose of 8.0 mg/kg) once weekly. Mice are treated with conventional doxorubicin at 4.0 and 8.0 mg/kg once weekly. For the LAGκ-2 experiment, Aldoxorubicin (INNO-206) is administered once weekly (W) at doses of 2.7 and 5.4 mg/kg, or on 3 consecutive days (W-F) weekly at doses of 0.9 and 1.8 mg/kg. PS-341 is administered twice weekly (W, F) at a dose of 0.5 mg/kg. Doxorubicin is administered to SCID mice at 2, 4, and 8 mg/kg, and PLD is administered to SCID mice at 2 mg/kg once weekly. Each drug is administered i.v. in a volume of 100 μL.[1-4]
数据来源文献[1]. Eric Sanchez, et al. Anti-Myeloma Effects of the Novel Anthracycline Derivative INNO-206. Clin Cancer Res.2012 18; 3856.
[2]. Kratz, F. INNO-206 (DOXO-EMCH), an Albumin-Binding Prodrug of Doxorubicin Under Development for Phase II Studies. Current Bioactive Compounds, 2011, 7(1): 33-38(6)
[3]. Graeser R, et al. INNO-206, the (6-maleimidocaproyl hydrazone derivative of doxorubicin), shows superior antitumor efficacy compared to doxorubicin in different tumor xenograft models and in an orthotopic pancreas carcinoma model. Invest New Drugs. 2010 F
[4]. Walker L, et al. Cell penetrating peptides fused to a thermally targeted biopolymer drug carrier improve the delivery and antitumor efficacy of an acid-sensitive doxorubicin derivative. Int J Pharm. 2012 Oct 15;436(1-2):825-32.
单位
1mM-5mg6.66mL
1mM-1mg1.332mL
1mM-10mg13.32mL
5mM-1mg0.2664mL
5mM-5mg1.332mL
5mM-10mg2.664mL
10mM-1mg0.1332mL
10mM-5mg0.666mL
10mM-10mg1.332mL
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