生物活性 靶点 体外研究 体内研究
ChemicalBook  CAS数据库列表  180084-26-8

180084-26-8

180084-26-8,180084-26-8,结构式
180084-26-8
  • CAS号:180084-26-8
  • 英文名:SB 224289 HYDROCHLORIDE
  • 中文名:180084-26-8
  • CBNumber:CB6972578
  • 分子式:C32H32N4O3HCl
  • 分子量:0
  • MOL File:180084-26-8.mol
180084-26-8化学性质
  • 储存条件 :Store at RT
  • 溶解度 :Soluble to 10 mM in DMSO with gentle warming
  • 形态 :Powder
  • 颜色 :White to off-white
安全信息

180084-26-8性质、用途与生产工艺

  • 生物活性 SB-224289 hydrochloride 是一种选择性的 5-HT1B receptor 拮抗剂,具有抗焦虑作用。
  • 靶点

    5-HT 1B Receptor

  • 体外研究

    SB-224289 has specific toxin-blocking ability and does not inhibit Cho1p. SB-224289 (100 μM-25 μM) shows consistent efficacy at producing Pap-A resistance. SB-224289 does not directly inhibit the PS synthase enzyme in this in vitro assay. Moreover, SB-224289 specifically blocks the activity of papuamides and not other membrane disruptors. SB-224289 is unable to protect wild-type cells against KF, but it is able to provide protection against TPap-A. SB-224289 has a pK i of 8 at human cloned 5-HT1B receptors and displays more than 80 fold selectivity over the closely related 5-HT1D receptor and a range of other receptors. SB-224289 is a potent antagonist with pEC 50 of 7.9±0.1. SB-224289 evokes a parallel rightward shift in the 5-HT concentration response curve with pA2 of 8.4±0.2. SB-224289 (100 nM and 1 μM) also significantly increases [ 3 H]-5HT release in electrically stimulated guinea-pig brain cortex slices.

  • 体内研究

    SB-224289 (SB 224289) alone or in combination with cocaine, increases anxiety-like behavior. SB 224289 significantly reduces the amount of locomotor activity in the cocaine-treated rats. SB 224289-treated animals spend a significantly longer time in the corners than those treated with vehicle. SB 224289 is a potent antagonist with an ED 50 of 3.6 mg/kg, p.o in SK&F-99101-induced hypothermia in the guinea-pig. SB 224289 (4 mg/kg, p.o) reverses sumatriptan-induced inhibition of 5-HT release showing that it is also a potent terminal 5-HT autoreceptor antagonist in vivo. SB 224289 (2-16 mg/kg, p.o) does not increase 5-HT levels in the fuinea-pig frontal cortex. However, SB 224289 (4 mg/kg, p.o) causes a significantly increase in levels of 5-HT in the fuinea-pig dentate gyrus.

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