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- 文献和实验
- 技术资料
- 保存条件:
Powder:2-8℃,2 years;Insolvent(母液):-20℃,6 months;-80℃,1 year
- 保质期:
Powder:2-8℃,2 years;Insolvent(母液):-20℃,6 months;-80℃,1 year
- 英文名:
Sunitinib
- 库存:
现询
- 供应商:
北京索莱宝科技有限公司
- CAS号:
557795-19-4
- 规格:
10mg/50mg/200mg/100mg/10mM*1mL in DMSO
| 规格: | 10mg | 产品价格: | ¥230.0 |
|---|---|---|---|
| 规格: | 50mg | 产品价格: | ¥460.0 |
| 规格: | 200mg | 产品价格: | ¥940.0 |
| 规格: | 100mg | 产品价格: | ¥640.0 |
| 规格: | 10mM*1mL in DMSO | 产品价格: | ¥500.0 |
是一种多靶点受体酪氨酸激酶抑制剂,抑制VEGFR2 和 PDGFRβ 。
【本资料源自公开渠道,如需(此处)屏蔽,请联系删除】
标题:OAS1 suppresses African swine fever virus replication by recruiting TRIM21 to degrade viral major capsid protein
成员:Hualin Sun, Mengli Wu, Zhonghui Zhang, Yiwang Wang, Jifei Yang, Zhijie Liu, Guiquan Guan, Jianxun Luo, Hong Yin, Qingli Niu
论文因子:5.4 发表期刊:JOURNAL OF VIROLOGY pmid:37815352
| 基本信息 | |
| CAS | No.557795-19-4 |
| 中文名称 | 舒尼替尼 |
| 英文名称 | Sunitinib |
| 别名 | SU11248 |
| 分子式 | C22H27FN4O2 |
| 分子量 | 398.47 |
| 溶解性 | Soluble in DMSO ≥25mg/mL |
| 纯度 | HPLC≥98% |
| 外观(性状) | Light yellow to yellow Solid |
| 储存条件 | Powder:2-8℃,2 years;Insolvent(母液):-20℃,6 months;-80℃,1 year |
| MDL | MFCD08273555 |
| SMILES | O=C(NCCN(CC)CC)C1=C(NC(/C=C2C(NC3=C\2C=C(C=C3)F)=O)=C1C)C |
| 靶点 | VEGFR;PDGFRβ |
| 通路 | Angiogenesis;Protein Tyrosine Kinase/RTK |
| 背景说明 | Sunitinib是一种多靶点受体酪氨酸激酶抑制剂,抑制VEGFR2 和 PDGFRβ 。 |
| 生物活性 | Sunitinib (SU 11248) is a multi-targeted receptor tyrosine kinase inhibitor with IC50s of 80 nM and 2 nM for VEGFR2 and PDGFRβ, respectively[1]. Sunitinib, an ATP-competitive inhibitor, effectively inhibits autophosphorylation of Ire1α by inhibiting autophosphorylation and consequent RNase activation[2]. |
| In Vitro | Sunitinib Malate is also a good inhibitor of KIT and FLT-3[1]. In RS4;11 cells(FLT3-WT),treatment with Sunitinib(SU11248)inhibits FLT3-WT phosphorylation in a dose-dependent manner with IC50 of approximately 250 nM. In MV4;11 cells that express FLT3-ITD,Sunitinib inhibits FLT3-ITD phosphorylation in a dose-dependent manner with an IC50 of 50 nM following a 2-hour treatment[3].In biochemical assays,Sunitinib(SU11248)exhibits competitive inhibition(with regard to ATP)against Flk-1 and PDGFRβ with Ki values of 9 nM and 8 nM,respectively. Sunitinib is also a competitive,albeit less potent,inhibitor of FGFR1 tyrosine kinase activity,with a Ki value of 0.83 μM. In addition to these three structurally related split kinase domain RTKs,the activity of Sunitinib has also been evaluated against a broad panel of additional tyrosine and serine/threonine kinases. In these biochemical assays,the IC50 values for Sunitinib are generally at least 10-fold higher than those for Flk-1 and PDGFR(e.g.,IC50values of: >10 μM for EGFR and Cdk2; 4 μM for Met; 2.4 μM for IGFR-1; 0.8 μM for Abl; and 0.6 μM for Src)[4]. |
| 细胞实验 | Sunitinib Malate has very good oral bioavailability,is highly efficacious in a number of preclinical tumor models,and is well tolerated at efficacious doses[1]. Sunitinib(80 mg/kg/day)inhibits the growth of established SF763T and Colo205 tumor xenografts in athymic mice. Sunitinib(SU11248)treatment effectively inhibits the growth of established tumor xenografts[4]. |
| 细胞实验 | RS4;11 and MV4;11 cell lines are starved overnight in medium containing 0.1% FBS prior to addition of Sunitinib(1 nM,5 nM,10 nM,25 nM,75 nM,100 nM,250 nM,500 nM)and FL(50 ng/mL; FLT3-WT cells only). Proliferation is measured after 48 hours of culture using the Alamar Blue assay in triplicate for each condition,as described by the manufacturer. Trypan blue cell viability assays are performed in parallel and yielded similar results[3]. |
| 动物实验 | Mice[2] Female nu/nu mice(8-12 weeks old,25 grams)are used. Briefly,3-5×106 tumor cells are implanted s.c. into the hind flank region of mice on day 0. Daily treatment of tumor-bearing mice with oral administration of Sunitinib as a carboxymethyl cellulose suspension or as a citrate buffered(pH 3.5)solution is initiated once the tumors reached the indicated average size. Tumor growth is evaluated based on twice-weekly measurement of tumor volume. Typically,studies are terminated when tumors in vehicle-treated animals reach an average size of 1000 mm3 or when the tumors are judged to adversely effect the well being of the animals. Rats[4] Adult male Wistar rats(325-349 g)are used. To validate the ability of the time-lapse imaging method to evaluate the anti-angiogenic effects for a given drug treatment,two drug studies are conducted. In the first study,mesenteric windows are harvested from adult male Wistar rats and cultured for 3 days according to the two experimental groups: 1)10% serum(n=8 tissues from 4 rats),and 2)10% serum+Sunitinib(5 μM; n=8 tissues from 4 rats). |
| 数据来源文献 | [1]. Sun L, et al. Discovery of 5-[5-fluoro-2-oxo-1,2- dihydroindol-(3Z)-ylidenemethyl]-2,4- dimethyl-1H-pyrrole-3-carboxylic acid (2-diethylaminoethyl)amide, a novel tyrosine kinase inhibitor targeting vascular endothelial and platelet-derived growth factor receptor tyrosine kinase. J Med Chem. 2003 Mar 27;46(7):1116-9. [2]. Ali MM, et al. Structure of the Ire1 autophosphorylation complex and implications for the unfolded protein response. EMBO J. 2011 Mar 2;30(5):894-905. [3]. O'Farrell AM, et al. SU11248 is a novel FLT3 tyrosine kinase inhibitor with potent activity in vitro and in vivo. Blood. 2003 May 1;101(9):3597-605. [4]. Mendel DB, et al. In vivo antitumor activity of SU11248, a novel tyrosine kinase inhibitor targeting vascular endothelial growth factor and platelet-derived growth factor receptors: determination of a pharmacokinetic/pharmacodynamic relationship. Clin Can |
| 单位 | 支 |
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【本资料源自公开渠道,如需(此处)屏蔽,请联系删除】
标题:OAS1 suppresses African swine fever virus replication by recruiting TRIM21 to degrade viral major capsid protein
成员:Hualin Sun, Mengli Wu, Zhonghui Zhang, Yiwang Wang, Jifei Yang, Zhijie Liu, Guiquan Guan, Jianxun Luo, Hong Yin, Qingli Niu
论文因子:5.4 发表期刊:JOURNAL OF VIROLOGY pmid:37815352
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