购物车 
-
帕苯咪唑
- names:
Parbendazole
- CAS号:
14255-87-9
MDL Number: MFCD00864534 - MF(分子式): C13H17N3O2 MW(分子量): 247.29
- EINECS:238-133-3 Reaxys Number:14255-87-9
- Pubchem ID:26596 Brand:BIOFOUNT
| 货品编码 | 规格 | 纯度 | 价格 (¥) | 现价(¥) | 特价(¥) | 库存描述 | 数量 | 总计 (¥) |
|---|---|---|---|---|---|---|---|---|
| YZM000773-25mg | 25mg | >98.0% | ¥ 810.00 | ¥ 810.00 | 2-3天 | ¥ 0.00 | ||
| YZM000773-10mg | 10mg | >98.0% | ¥ 487.50 | ¥ 487.50 | 2-3天 | ¥ 0.00 |
| 中文别名 | 帕苯咪唑(Parbendazole,14255-87-9) |
| 英文别名 | Parbendazole(帕苯咪唑,14255-87-9) |
| CAS号 | 14255-87-9 |
| SMILES | O=C(OC)NC1=NC2=CC=C(CCCC)C=C2N1 |
| Inchi | InChI=1S/C13H17N3O2/c1-3-4-5-9-6-7-10-11(8-9)15-12(14-10)16-13(17)18-2/h6-8H,3-5H2,1-2H3,(H2,14,15,16,17) |
| InchiKey | YRWLZFXJFBZBEY-UHFFFAOYSA-N |
| 分子式 Formula | C13H17N3O2 |
| 分子量 Molecular Weight | 247.29 |
| 闪点 FP | |
| 熔点 Melting point | 255-257°C |
| 沸点 Boiling point | 390.33°C (rough estimate) |
| Polarizability极化度 | 28.3±0.5 10-24cm3 |
| 密度 Density | 1.2±0.1 g/cm3 |
| 蒸汽压 Vapor Pressure | 28.3±0.5 10-24cm3 |
| 溶解度Solubility | 生物体外In Vitro:DMSO溶解度4 mg/mL(16.18 mM;Need ultrasonic)H2O< 0.1 mg/mL(insoluble) |
| 性状 | 固体粉末,Power |
| 储藏条件 Storage conditions | -20°C 3 years年 4°C 2 years年 / In solvent溶液中:-80°C 6 months月 -20°C 1 month月 |
| 生物 | 测试类型 | 路线 | 报告剂量(标准化剂量) | 影响 | 参考 |
| cattle | LD | unreported | > 1200mg/kg (1200mg/kg) | Australian Veterinary Journal. Vol. 46, Pg. 297, 1970. | |
| chicken | LD50 | oral | > 40mg/kg (40mg/kg) | United States Patent Document. Vol. #3657267, | |
| domestic animals - goat/sheep | LDLo | oral | 660mg/kg (660mg/kg) | GASTROINTESTINAL: ULCERATION OR BLEEDING FROM STOMACH | Australian Veterinary Journal. Vol. 46, Pg. 297, 1970. |
| mouse | LD50 | oral | 1700mg/kg (1700mg/kg) | Bulletin de la Societe des Sciences Veterinaires et de Medecine Comparee de Lyon. Vol. 77, Pg. 379, 1975. | |
| rat | LD50 | oral | > 40mg/kg (40mg/kg) | United States Patent Document. Vol. #3657267, |
帕苯咪唑(Parbendazole,14255-87-9)物理性质:
| 物理属性 | 值 | 单位 | 温度(摄氏度) | 资源 |
| Melting Point | 226 dec | deg C | EXP | |
| log P (octanol-water) | 3.570 | (none) | EST | |
| Atmospheric OH Rate Constant | 2.05E-10 | cm3/molecule-sec | 25 | EST |
帕苯咪唑(Parbendazole,14255-87-9)实验注意事项:
1.实验前需戴好防护眼镜,穿戴防护服和口罩,佩戴手套,避免与皮肤接触。
2.实验过程中如遇到有毒或者刺激性物质及有害物质产生,必要时实验操作需要手套箱内完成以免对实验人员造成伤害
3.实验后产生的废弃物需分类存储,并交于专业生物废气物处理公司处理,以免造成环境污染Experimental considerations:
1. Wear protective glasses, protective clothing and masks, gloves, and avoid contact with the skin during the experiment.
2. The waste generated after the experiment needs to be stored separately, and handed over to a professional biological waste gas treatment company to avoid environmental pollution.
Tag:帕苯咪唑(MSDS,帕苯咪唑(蒸汽压,帕苯咪唑(合成,帕苯咪唑(标准,帕苯咪唑(应用,帕苯咪唑(合成,帕苯咪唑(沸点,帕苯咪唑(闪点,帕苯咪唑(用途,帕苯咪唑(溶解度,帕苯咪唑(价格,帕苯咪唑(作用,帕苯咪唑(结构式,帕苯咪唑(用处,帕苯咪唑(毒理性质,帕苯咪唑(物理性质)
| 产品说明 | 帕苯咪唑(Parbendazole,14255-87-9)是一种有效的microtubule重组的抑制剂,能够破坏微管蛋白,EC50值是 8.79nM,具有广谱的驱虫作用 |
| Introduction | Parbendazole(帕苯咪唑,14255-87-9)Parbendazole is a potent inhibitor of microtubuleassembly, destabilizes tubulin, with anEC50of 8.79nM, and exhibits a broadpectrum anthelmintic activity. |
| Application1 | |
| Application2 | |
| Application3 |
| 警示图 | |
| 危险性 | warning |
| 危险性警示 | Not available |
| 安全声明 | H303吞入可能有害+H313皮肤接触可能有害+H2413吸入可能对身体有害 |
| 安全防护 | P264处理后彻底清洗+P280戴防护手套/穿防护服/戴防护眼罩/戴防护面具+P305如果进入眼睛+P351用水小心冲洗几分钟+P338取出隐形眼镜(如果有)并且易于操作,继续冲洗+P337如果眼睛刺激持续+P2393获得医疗建议/护理 |
| 备注 | 实验过程中防止吸入、食入,做好安全防护 |
| Niche-based screening identifies small-molecule inhibitors of leukemia stem cells. Nature Chemical Biology 2013 |
| Chemotherapy of Gastrointestinal Nematodiasis in Ruminants Chemotherapy of Gastrointestinal Helminths 1985 |
| Molecular and Cellular Aspects of the Interaction of Benzimidazole Carbamate Pesticides with Microtubules The Cytoskeleton 1986 |
| Identification of biliary metabolites of Mebendazole in the rat European Journal of Drug Metabolism and Pharmacokinetics 1982 |
| Chemotherapeutic approaches to nematodes: current knowledge and outlook Parasitology Research/2001 |
Niche-based screening identifies small-molecule inhibitors of leukemia stem cells
Abstract
Efforts to develop more effective therapies for acute leukemia may benefit from high-throughput screening systems that reflect the complex physiology of the disease, including leukemia stem cells (LSCs) and supportive interactions with the bone marrow microenvironment. The therapeutic targeting of LSCs is challenging because LSCs are highly similar to normal hematopoietic stem and progenitor cells (HSPCs) and are protected by stromal cells in vivo. We screened 14,718 compounds in a leukemia-stroma co-culture system for inhibition of cobblestone formation, a cellular behavior associated with stem-cell function. Among those compounds that inhibited malignant cells but spared HSPCs was the cholesterol-lowering drug lovastatin. Lovastatin showed anti-LSC activity in vitro and in an in vivo bone marrow transplantation model. Mechanistic studies demonstrated that the effect was on target, via inhibition of HMG-CoA reductase. These results illustrate the power of merging physiologically relevant models with high-throughput screening.
Quantitative high-throughput profiling of environmental chemicals and drugs that modulate farnesoid X receptor
Abstract
The farnesoid X receptor (FXR) regulates the homeostasis of bile acids, lipids, and glucose. Because endogenous chemicals bind and activate FXR, it is important to examine which xenobiotic compounds would disrupt normal receptor function. We used a cell-based human FXR β-lactamase (Bla) reporter gene assay to profile the Tox21 10K compound collection of environmental chemicals and drugs. Structure-activity relationships of FXR-active compounds revealed by this screening were then compared against the androgen receptor, estrogen receptor α, peroxisome proliferator-activated receptors δ and γ, and the vitamin D receptor. We identified several FXR-active structural classes including anthracyclines, benzimidazoles, dihydropyridines, pyrethroids, retinoic acids, and vinca alkaloids. Microtubule inhibitors potently decreased FXR reporter gene activity. Pyrethroids specifically antagonized FXR transactivation. Anthracyclines affected reporter activity in all tested assays, suggesting non-specific activity. These results provide important information to prioritize chemicals for further investigation, and suggest possible modes of action of compounds in FXR signaling.
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