生物活性 靶点 体外研究 体内研究
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CIPEMASTAT

CIPEMASTAT,190648-49-8,结构式
CIPEMASTAT
  • CAS号:190648-49-8
  • 英文名:Ro 32-3555
  • 中文名:CIPEMASTAT
  • CBNumber:CB61394281
  • 分子式:C22H36N4O5
  • 分子量:436.54504
  • MOL File:190648-49-8.mol
CIPEMASTAT化学性质
  • 熔点 :>156°C (Dec.)
  • 密度 :1.205±0.06 g/cm3(Predicted)
  • 储存条件 :Store at -20°C
  • 溶解度 :Chloroform (Slightly), Methanol (Slightly)
  • 形态 :Solid
  • 酸度系数(pKa) :9.16±0.40(Predicted)
  • 颜色 :Light Beige to Beige

CIPEMASTAT性质、用途与生产工艺

  • 生物活性 Cipemastat 是一种有效的、人胶原酶 (collagenase) 1,2,3的抑制剂,其 Ki 值分别为 3.0,4.4,3.4 nM。
  • 靶点

    collagenases 1

    3.0 nM (Ki)

    collagenases 2

    4.4 nM (Ki)

    collagenases 3

    3.4 nM (Ki)

    stromelysins 1

    527 nM (Ki)

    gelatinase A

    154 nM (Ki)

    gelatinase B

    59.1 nM (Ki)

  • 体外研究

    Cipemastat (Ro 32-3555) is a potent, competitive inhibitor of human matrix metalloproteinases. Cipemastat is selective for collagenase 1, 2 and 3 relative to related matrix metalloproteinases. Cipemastat is also a potent inhibitor of rat collagenase (IC 50 =44.7±3.4 nM (n=4)). In vitro cartilage degradation ± inhibited IL-1a induced cartilage degradation in vitro in a concentration-dependent manner with an IC 50 =60 nM. The inhibition is not mediated by a cytotoxic action on explant chondrocytes. Cipemastat, at all concentrations tested, fail to modify glucose utilization when compared to explants cultured in the presence of IL-La alone.

  • 体内研究

    The amount of hydroxyproline in non-implanted cartilage is 119.3±4.2 nM/mg and this decreases in cartilages implanted in vehicle-dosed animals to 53.6±7.1 nM/mg over a fourteen day period. Animals administered Cipemastat orally at doses of 2.5, 5, 10 and 25 mg/kg show statistically increased levels of implanted cartilage hydroxypro-line. Fourteen days after the second challenge injection of P. acnes , the area of cartilage most consistently affected by pannus is the lateral femoral condyle, which is the area analysed. In non-arthritic animals the mean cartilage area is 0.17±0.02 mm 2 (n=5). In arthritic animals there is a significant decrease to a mean area of 0.086±0.01 mm 2 (n=10). The group of animals dosed with Cipemastat (50 mg/kg, p.o.) show a significantly greater area of cartilage with a mean value of 0.126±0.012 mm 2 (n=9). The pannus area in vehicle-dosed animals is 0.099±0.017 mm 2 and in Cipemastat dosed animals 0.102±0.019 mm 2 . Adjuvant arthritis injection of adjuvant induced two phases of swelling of the injected paw in vehicle-dosed rats. The primary swelling phase occurred between days 0 to 5 and induced an increase in paw volume of 1.9±0.1 mL; the secondary phase occurrs between day 9 to 14 and there was an increase in paw swelling of 0.98±0.08 mL. The group of animals dosed with dexamethasone (0.1 mg/kg) shows a significant reduction in both primary (0.2±0.03 mL) and secondary inflammation (0.07±0.08 mL) paw swelling as well as total inhibition of the lesion score.

CIPEMASTAT上下游产品信息
上游原料
下游产品
CIPEMASTAT生产厂家
  • 公司名称:北京华美互利生物化工
  • 联系电话:010-56205725
  • 电子邮件:waley188@sohu.com
  • 国家:中国
  • 产品数:12338
  • 优势度:58
  • 公司名称:上海喀露蓝科技有限公司
  • 联系电话: 18149758185
  • 电子邮件:sales-cpd@caerulumpharma.com
  • 国家:中国
  • 产品数:3465
  • 优势度:58
  • 公司名称:上海传芊化工科技中心
  • 联系电话: 15869524721
  • 电子邮件:3525679403@qq.com
  • 国家:中国
  • 产品数:3721
  • 优势度:58
  • 公司名称:TargetMol中国(陶术生物)
  • 联系电话: 4008200310
  • 电子邮件:marketing@tsbiochem.com
  • 国家:中国
  • 产品数:23963
  • 优势度:58