生物活性 靶点 体外研究 体内研究
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H-THR-PHE-LEU-LEU-ARG-NH2

H-THR-PHE-LEU-LEU-ARG-NH2,197794-83-5,结构式
H-THR-PHE-LEU-LEU-ARG-NH2
  • CAS号:197794-83-5
  • 英文名:TFLLR-NH2
  • 中文名:H-THR-PHE-LEU-LEU-ARG-NH2
  • CBNumber:CB9464681
  • 分子式:C31H53N9O6
  • 分子量:647.81
  • MOL File:197794-83-5.mol
H-THR-PHE-LEU-LEU-ARG-NH2化学性质
  • 密度 :1.31±0.1 g/cm3(Predicted)
  • 储存条件 :Desiccate at -20°C
  • 酸度系数(pKa) :12.10±0.45(Predicted)
  • 形态 :Powder
  • 水溶解性 :Soluble to 1 mg/ml in water

H-THR-PHE-LEU-LEU-ARG-NH2性质、用途与生产工艺

  • 生物活性 TFLLR-NH2是选择性的PAR1激动剂,EC50值为1.9 μM。
  • 靶点

    EC50: 1.9 μM (PAR1)

  • 体外研究

    PAR1 agonists stimulate concentration-dependent increases in [Ca 2+ ]i and in the proportions of neurones. The maximal increase in [Ca 2+ ]i above basal is detected in response to 10 μm TF-NH2(peak 196.5±20.4 nM, n=25) when 50–80% of identified neurones responded. SW620 cells cultured in the supernatant of TFLLR-NH2-activated platelets upregulate E-cadherin expression and downregulate the vimentin expression. In the in vitro platelet culture system, a TFLLR-NH2 dose-dependent increase of secreted TGF-β1 is detected in the supernatant.

  • 体内研究

    Injection of TF-NH2 into the rat paw stimulates a marked and sustained oedema. An NK1R antagonist and ablation of sensory nerves with capsaicin inhibit oedema by 44% at 1 h and completely by 5 h. In wild-type but not PAR1 −/− mice, TF-NH2 stimulates Evans blue extravasation in the bladder, oesophagus, stomach, intestine and pancreas by 2–8 fold. Extravasation in the bladder, oesophagus and stomach is abolished by an NK1R antagonist. TFp-NH2 produces notable contraction at 3-50 μM and relaxation at 0.3-50 μM, in the absence of apamin. The concentration-response curve for TFp-NH2-induced contraction is remarkably shifted left, when the TFp-NH2-induced relaxation is blocked by apamin at 0.1 μM.

H-THR-PHE-LEU-LEU-ARG-NH2上下游产品信息
上游原料
下游产品
H-THR-PHE-LEU-LEU-ARG-NH2生产厂家
  • 公司名称:Labinova AB
  • 联系电话:--
  • 电子邮件:info@labinova.se
  • 国家:欧洲
  • 产品数:281
  • 优势度:64
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