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(S)-( )-Ibuprofen

CAS No. 51146-56-6

(S)-( )-Ibuprofen ( S)-Ibuprofen )

产品货号. M14764 CAS No. 51146-56-6

布洛芬的一种对映体,比 (R) 型更能有效地抑制 COX 活性、血栓素形成和血小板聚集。

纯度: >98% (HPLC)

COA Datasheet HNMR HPLC MSDS Handing Instructions
规格 价格/人民币 库存 数量
500MG 获取报价 有现货
1G ¥111 有现货

生物学信息

  • 产品名称
    (S)-( )-Ibuprofen
  • 注意事项
    本公司产品仅用于科研实验,不得用于人体或动物的临床与诊断
  • 产品简述
    布洛芬的一种对映体,比 (R) 型更能有效地抑制 COX 活性、血栓素形成和血小板聚集。
  • 产品描述
    An enantiomer of Ibuprofen that more potently inhibits COX activity, thromboxane formation, and platelet aggregation than the (R)-form; also inhibits activation of NF-κB more effectively than (R)-ibuprofen (IC50=62 and 122 uM, respectively).(In Vitro):(S)-(+)-Ibuprofen (HCT-15 and HCA-7 cells; 0-1000 μM; 8 days) treatment reduces concentration dependently cell survival in both cell lines to a similar extent.(S)-(+)-Ibuprofen (HCT-15 and HCA-7 cells; 0-1000 μM; 20-72 hours) treatment causes a G0/G1 phase block as well as apoptosis.(S)-(+)-Ibuprofen (HCT-15 and HCA-7 cells; 900 μM; 4-72 hours) treatment shows a down regulation of cyclin A and B and an increase of the cell cycle inhibitory protein p27Kip-1.(S)-(+)-Ibuprofen inhibits COX activity, thromboxane formation, and platelet aggregation.(S)-(+)-Ibuprofen inhibits the activation of NF-κB in response to T-cell stimulation with an IC50 of 61.7 μM.(In Vivo):(S)-(+)-Ibuprofen (15 mg/kg/day; intraperitoneal injection; five days a week; for 4 weeks) treatment inhibits tumor growth of HCA-7 and HCT-15 xenografts in the nude mice model.
  • 体外实验
    (S)-(+)-Ibuprofen (HCT-15 and HCA-7 cells; 0-1000 μM; 8 days) treatment reduces concentration dependently cell survival in both cell lines to a similar extent. (S)-(+)-Ibuprofen (HCT-15 and HCA-7 cells; 0-1000 μM; 20-72 hours) treatment causes a G0/G1 phase block as well as apoptosis.(S)-(+)-Ibuprofen (HCT-15 and HCA-7 cells; 900 μM; 4-72 hours) treatment shows a down regulation of cyclin A and B and an increase of the cell cycle inhibitory protein p27Kip-1. (S)-(+)-Ibuprofen inhibits COX activity, thromboxane formation, and platelet aggregation.(S)-(+)-Ibuprofen inhibits the activation of NF-κB in response to T-cell stimulation with an IC50 of 61.7 μM. Cell Proliferation Assay Cell Line:HCT-15 and HCA-7 cells Concentration:0 μM, 200 μM, 400 μM, 600 μM, 700 μM, 800 μM, 900 μM, and 1000 μM Incubation Time:8 days Result:Reduced concentration dependently cell survival in both cell lines to a similar extent.Cell Cycle Analysis Cell Line:HCT-15 and HCA-7 cells Concentration:0 μM, 200 μM, 400 μM, 600 μM, 800 μM, 900 μM, and 1000 μM Incubation Time:24 hours (HCT-15) or 20 hours (HCA-7)Result:Caused a G0/G1 phase block.Apoptosis Analysis Cell Line:HCT-15 and HCA-7 cells Concentration:0 μM, 200 μM, 400 μM, 600 μM, 800 μM, 900 μM, and 1000 μM Incubation Time:72 hours Result:Induced cell apoptosis.Western Blot Analysis Cell Line:HCT-15 and HCA-7 cells Concentration:900 μM Incubation Time:4 hours, 8 hours, 16 hours, 24 hours, 32 hours, 48 hours and 72 hours Result:Decreased levels of Cyclin D1 protein.
  • 体内实验
    (S)-(+)-Ibuprofen (15 mg/kg/day; intraperitoneal injection; five days a week; for 4 weeks) treatment inhibits tumor growth of HCA-7 and HCT-15 xenografts in the nude mice model. Animal Model:NMRI (nu/nu) male mice (6-8 week old ) injected with HCA-7 and HCT-15 cells Dosage:15 mg/kg/day Administration:Intraperitoneal injection; five days a week; for 4 weeks Result:Inhibited tumor growth of HCA-7 and HCT-15 xenografts in mice.
  • 同义词
    S)-Ibuprofen
  • 通路
    Chromatin/Epigenetic
  • 靶点
    COX
  • 受体
    Bcl-2|COX|Cysticfibrosistransmembraneconductanceregulator|PPARγ|thrombomodulin
  • 研究领域
    Inflammation/Immunology
  • 适应症
    ——

化学信息

  • CAS Number
    51146-56-6
  • 分子量
    206.2808
  • 分子式
    C13H18O2
  • 纯度
    >98% (HPLC)
  • 溶解度
    H2O: 1 mg/mL (Need ultrasonic and warming); DMSO: < 0.1 mg/mL
  • SMILES
    C[C@@H](C1=CC=C(C=C1)CC(C)C)C(=O)O
  • 化学全称
    Benzeneacetic acid, α-methyl-4-(2-methylpropyl)-,(αS)-

运输与储存

  • 储存条件
    (-20℃)
  • 运输条件
    With Ice Pack
  • 稳定性
    ≥ 2 years

参考文献

1. Evans AM, et al. Br J Clin Pharmacol. 1991 Feb;31(2):131-8. 2. Villanueva M, et al. Br J Clin Pharmacol. 1993 Mar;35(3):235-42. 3. Scheuren N, et al. Br J Pharmacol. 1998 Feb;123(4):645-52.
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