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  • 甲磺酸去铁胺|T1637|TargetMol

甲磺酸去铁胺|T1637|TargetMol

Deferoxamine Mesylate
138-14-7
99 5mg 起订
129 10mg 起订
193 25mg 起订
上海 更新日期:2024-09-23

TargetMol中国(陶术生物)

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产品详情:

中文名称:
甲磺酸去铁胺
英文名称:
Deferoxamine Mesylate
CAS号:
138-14-7
品牌:
TargetMol
产地:
美国
保存条件:
store at low temperature,keep away from direct sunlight | Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
纯度规格:
99.80%
产品类别:
抑制剂
货号:
T1637

Product Introduction

Bioactivity

名称Deferoxamine Mesylate
描述Deferoxamine Mesylate (DFOM) is an iron chelator and ferroptosis inhibitor. Deferoxamine Mesylate binds free iron into a stable complex and reduces iron accumulation. Deferoxamine Mesylate up-regulates HIF-1α levels and induces apoptosis.
细胞实验After cells were seeded onto the collagen-GAG discs and allowed to adhere for 3?hours, they were placed into a hypoxic incubator with 1% O2 or incubated under standard cell culture conditions with deferoxamine mesylate (DFO) added to final concentrations of 30, 60, or 120?μM. Scaffolds seeded with AdMSCs cultured under standard conditions were used as a control [3].
动物实验The animals were divided into 4 groups: sham, SAH, SAH+vehicle and SAH+DFX (100mg/kg) group. DFX was administered intraperitoneally 2 and 6 hours after hemorrhage followed by every 12 hours for a maximum of 7 days. The same time course and dosage of saline were administered in the SAH+vehicle group. Afterward, rats underwent behavioral testing and were euthanized at day 1, 3, 7 and 28 for brain water content calculation, immunohistochemistry or western blot assays. The study was performed in three parts. Part 1 measured the brain water content, Evan's blue extravasation, and ultrastructural abnormalities at day 1, 3 and 7 after SAH to evaluate the time-dependent changes in brain edema and BBB disruption (n = 4 per time point and group). Part 2 investigated the role of iron in SAH-induced BBB disruption at day 1, 3 and 7 by brain water content (n = 4, per time point and group), Evan's blue extravasation (n = 4, per time point and group), transmission electron microscopy (n = 4, per time point and group), immunohistochemistry (n = 4, per time point and group) and western blot analysis (n = 3, per time point and group). Part 3 compared the acute (n = 61, per group at day 1; n = 42, per group at day 3; n = 23, per group at day 7) and long term (n = 4, per group at day 28) neurological function after SAH in each group to determine the effect of iron chelation on SAH-induced neurologic impairment [4].
体外活性方法:人宫颈癌细胞 HeLa 用 Deferoxamine Mesylate (3-100 μM) 处理 72 h,使用 Incucyte HD imaging system 检测细胞数目。 结果:Deferoxamine Mesylate 以浓度依赖的方式抑制细胞生长,在100 μM 下观察到显著的生长抑制。[1] 方法:人结直肠癌细胞 HT29 和 HCT116 用 Deferoxamine Mesylate (50-200 μM) 处理 48 h,使用 Western Blot 方法检测靶点蛋白表达水平。 结果:Deferoxamine Mesylate 以剂量依赖性方式诱导 HIF-1α 的显著表达。[2] 方法:人乳腺癌细胞 MDA-MB-231 和 MCF-7 用 Deferoxamine Mesylate (200 μM) 处理 24 h,使用 Flow Cytometry 方法检测细胞凋亡情况。 结果:Deferoxamine Mesylate 处理后,与未处理的细胞相比,MDA-MB-231 细胞的凋亡率没有变化,而 MCF-7 细胞的凋亡显著增加。[3]
体内活性方法:为研究 Deferoxamine Mesylate 是否能减轻实验小鼠的炎症和动脉粥样硬化,将 Deferoxamine Mesylate (100 mg/kg) 腹腔注射给载脂蛋白 E 缺陷 (apoE-/-) 小鼠,每天一次,持续十周。 结果:Deferoxamine Mesylate 使主动脉动脉粥样硬化病变的发展减少 26%。Deferoxamine Mesylate 还降低了血清 MCP-1 水平以及主动脉和心脏中促炎和巨噬细胞标志物的基因表达,同时增加了心脏和肝脏中转铁蛋白受体的蛋白质表达。相反,Deferoxamine Mesylate 治疗对血清胆固醇和甘油三酯水平没有影响。[4] 方法:为研究 Deferoxamine Mesylate 对 ob/ob 小鼠附睾脂肪组织中脂肪细胞功能障碍的影响,将 Deferoxamine Mesylate (100 mg/kg) 腹腔注射给 ob/ob 小鼠,每天一次,持续十五天。 结果:Deferoxamine Mesylate 通过减少活性氧和炎症标志物的分泌,通过增加抗氧化酶、HIF-1α 和 HIF-1α 靶向蛋白的水平,以及通过改变脂肪细胞铁、葡萄糖和脂质相关代谢蛋白,显著改善了脂肪组织生物学的重要参数。同时,Deferoxamine Mesylate 治疗后,肥大的脂肪细胞体积缩小,胰岛素信号通路相关蛋白也被激活。[5]
存储条件store at low temperature,keep away from direct sunlight | Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
溶解度DMSO : 152.3 mM
H2O : 20.83 mg/mL (31.72 mM)
关键字HIFs | neovascularization | TAMSCs | diabetes mellitus | Akt | Deferoxamine Mesylate | PKB | Protein kinase B | Apoptosis | Autophagy | SH-SY5Y | Hypoxia-inducible factors | Deferoxamine | Desferrioxamine B Mesylate | Inhibitor | MEFs | cancer | Alzheimer’s disease | HIF-PH | Reactive Oxygen Species | BMMSCs | inhibit | HIF/HIF Prolyl-Hydroxylase | COVID-19
相关产品L-Cystine | Guanidine hydrochloride | Naringin | Valproic Acid | L-Glutamic acid | Gefitinib | Aceglutamide | Hydroxychloroquine | Stavudine | Acetylcysteine | Paeonol | Sodium 4-phenylbutyrate
相关库抗癌上市药物库 | 经典已知活性库 | 抗衰老化合物库 | FDA 上市药物库 | 神经退行性疾病化合物库 | 药物功能重定位化合物库 | 抗癌临床化合物库
去铁铵|||甲磺酸去铁胺|||DFOM|||DFO|||Desferrioxamine B mesylate|||desferrioxamine B|TargetMol

公司简介

上海陶术生物科技有限公司为美国Target Molecule Corp. ( Target Mol ) 在上海建立的全资子公司。我们与美国波士顿、德国慕尼黑的同事一起,为北美、欧洲和亚洲从事药物研发和生物学研究的科学家提供优质的产品和专业的服务。公司下设筛选事业部,化学事业部,生物事业部和新材料部。 从虚拟筛选到实体化合物分子供应;从商业化产品销售到个性化定制合成;从对明确靶点的分子筛选到对明确分子的多靶点筛选,从高通量筛选到化学结构优化,我们都可以满足您的科研用品及技术服务的需求。 经过在中国市场五年的精心耕耘,我们已成为筛选化合物领域优秀的供应商,为超过五百家学校和各类企业提供了品质卓越的小分子化合物和药物筛

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主营行业 化学试剂,生物活性小分子

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