化合物 LY2109761,LY2109761
  • 化合物 LY2109761,LY2109761

化合物 LY2109761|T2123|TargetMol

4篇文献
价格 251 367 663
包装 1mg 2mg 5mg
最小起订量 1mg
发货地 上海
更新日期 2025-11-17
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产品详情

中文名称:化合物 LY2109761英文名称:LY2109761
CAS:700874-71-1品牌: TargetMol
产地: 美国保存条件: store at low temperature | Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice/Shipping at ambient temperature.
纯度规格: 99.64%产品类别: 抑制剂
货号: T2123
2025-11-17 化合物 LY2109761 LY2109761 1mg/251RMB;2mg/367RMB;5mg/663RMB 251 TargetMol 美国 store at low temperature | Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice/Shipping at ambient temperature. 99.64% 抑制剂

Product Introduction

Bioactivity

名称LY2109761
描述LY2109761 is a novel selective TGF-β receptor type I/II (TβRI/II) dual inhibitor with Ki of 38 nM and 300 nM, respectively; shown to negatively affect the phosphorylation of Smad2.
细胞实验LY2109761 cytotoxicity was determined by 3 methods: the MTT assay, manual counting of viable cells, and propidium iodide staining. MTT yields a purple formazan product that is detected using a 96-well plate reader at 570 nm. Cells were plated and cultured for 2 days in a 1% fetal bovine serum medium supplemented with LY2109761 at the following concentrations: 0.001, 0.01, 0.1, 1, 10, and 20 μM. Each experimental condition was reproduced in 8 wells, and each experiment was repeated 3 times. To confirm the cytotoxic data, cells were incubated under the described conditions and stained with the vital dye trypan blue, which does not react with the cell membrane because of its negative charge. All the unstained cells were counted using a hemocytometer. Four squares were counted for each condition, and each condition was repeated in triplicate in the same experiment. Each experiment was repeated 3 times for each cell line. Bars represent the average and standard deviation of all experiments. Under the same experimental conditions, nonpermeabilized cells were stained with propidium iodide and analyzed with a flow cytometer [2].
动物实验Three days after the orthotopic implantation of 1.0 × 106 L3.6pl/GLT tumor cells in 50 μL of HBSS, when bioluminescence imaging confirmed that tumors were well established, 40 mice were randomly allocated into four groups (n = 10 mice per group) to receive one of the following treatments. (a) Vehicle solution for 50 μL of LY2109761 twice a day p.o. (days 1–5 of each week) and 50 μL of sterile saline daily i.p. (days 2 and 5 of each week; control group). (b) LY2109761 (50 mg/kg) twice a day p.o. (days 1–5 of each week) and 50 μL of sterile saline daily i.p. (days 2 and 5 of each week). (c) Gemcitabine (25 mg/kg) daily i.p. (days 2 and 5 of each week) and p.o. vehicle for 50μL of LY2109761 twice a day (days 1–5 of each week). (d) LY2109761 (50 mg/kg) twice a day (days 1–5 of each week) and gemcitabine (25 mg/kg) daily i.p. (days 2 and 5 of each week). Treatments were continued for 4 wk. All mice were weighed weekly and observed for tumor growth. Tumor diameter was assessed with a Vernier caliper, and tumor volume (mm3) was calculated as d2 × D/2, wherein d and D represent the shortest and longest diameters, respectively. Bulky disease was considered present when the tumor burden was prominent in the mouse abdomen (tumor volume, ≥2,000 mm3). When at least 6 of 10 mice in a treatment group presented with bulky disease, the median survival duration for that group was considered to be reached. At the median survival duration of the control group, the tumor growth in mice in all groups was evaluated using the bioluminescence emitted by the tumor cells. Bioluminescence imaging was conducted using a cryogenically cooled IVIS 100 imaging system coupled to a data acquisition computer running Living Image software. The mice were sacrificed by carbon dioxide inhalation when evidence of advanced bulky disease was present. The day of sacrifice was considered the day of death for survival evaluation [1].
体外活性以LY2109761 (5 μM) 针对TβRI/II激酶活性几乎完全抑制了L3.6pl/GLT细胞的基础迁移率(P = 0.0107)及TGF-β1刺激下的迁移(P < 0.0001),表明L3.6pl/GLT细胞的体外迁移主要由内源性TGF-β驱动[1]。LY2109761 (0.001-0.1 μM) 显著上调E-cadherin mRNA及蛋白水平(P < 0.001),增加的E-cadherin主要定位于细胞膜,介导细胞间的锚定作用[2]。LY2109761 (10 μM) 或单独辐射 (4 Gy) 均能降低NMA-23细胞的神经球形成效率。LY2109761与辐射的联合应用在神经球形成和限制稀释实验中显示出超加性效应[3]。
体内活性LY2109761 (50 mg/kg, p.o.) 显著减小了肿瘤体积,并将小鼠的中位生存时间延长至45.0天,但差异并不显著。仅当LY2109761与gemcitabine联合使用时,肿瘤体积(P < 0.05)和中位生存时间显著受到影响,后者增加至77.5天(P = 0.0018) [1]。在一种原位颅内模型中,LY2109761显著减缓了肿瘤增长,延长了生存期,并延长了放射治疗引起的生存期延长。组织学分析表明,LY2109761抑制了放射促进的肿瘤侵袭,减少了肿瘤微血管密度,并减轻了间质转换 [3]。
存储条件store at low temperature | Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice/Shipping at ambient temperature.
溶解度10% DMSO+40% PEG300+5% Tween 80+45% Saline : 1 mg/mL (2.26 mM), Sonication is recommended.
DMSO : 6.88 mg/mL (15.58 mM), Sonication is recommended.
Ethanol : Insoluble
H2O : Insoluble
关键字TβRII | TβRI | Transforming growth factor beta receptors | TGF-β/Smad | TGF-β Receptor | TGFβ | TGFbeta/Smad | TGF-beta | TGFbeta | TGF-b/Smad | TGFb | Smad | LY-2109761 | LY2109761 | LY 2109761 | Inhibitor | inhibit | Autophagy
相关产品Oxyresveratrol | Guanidine hydrochloride | Naringin | Valproic Acid | Taurine | Gefitinib | Aceglutamide | Hydroxychloroquine | Curcumin | Stavudine | Paeonol | Sodium 4-phenylbutyrate
相关库抑制剂库 | 血管生成库 | 经典已知活性库 | 已知活性化合物库 | 激酶抑制剂库 | 抗衰老化合物库 | 抗肝癌化合物库 | 抗卵巢癌化合物库 | 抗COVID-19化合物库 | 癌细胞分化化合物库 | TGF-β/Smad靶点化合物库 | 膜蛋白靶向化合物库
关键字: LY2109761|TargetMol

公司简介

TargetMol Chemicals Inc. 总部位于马萨诸塞州波士顿,致力于为全球生化领域科学家的研究提供专业的产品和服务。TargetMol?品牌的客户群分布于40多个国家和地区,已发展成为全球知名的化合物库和小分子化合物研究供应商。 TargetMol?可提供160多种满足不同需求的化合物库,以及多种类型的生化试剂产品,包括12000多种抑制剂、16000多种天然产物和各类多肽、抗体、生命科学试剂盒等,此外,我们还建设有CADD(计算机辅助药物设计)研究中心、药理实验室、药化合成平台三大技术中心,全方位满足客户的定制需求。 凭借我们优质的产品和服务、快速高效的全球供应链和专业的技术支持,我们将有效帮助您缩短研发周期,取得更成功的结果。
成立日期 2013-04-18 (13年) 注册资本 566.265100万人民币
员工人数 100-500人 年营业额 ¥ 1亿以上
主营行业 天然产物,生化试剂,分子生物学,分子砌块,生物技术服务 经营模式 贸易,工厂,试剂,定制,服务
  • TargetMol中国(陶术生物)
VIP 4年
  • 公司成立:13年
  • 注册资本:566.265100万人民币
  • 企业类型:有限责任公司(自然人投资或控股)
  • 主营产品:小分子抑制剂、药物筛选化合物库、药物筛选等
  • 公司地址:静安区江场三路238号8楼
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