CasImg
小白菊内酯
产品纠错
CAS号:20554-84-1 | 英文名称:Parthenolide
分子式 C15H20O3
分子量 248
EINECS号 692-532-0
MDL MFCD00134592
Smiles
InChIKey
乙二醇化学百科
基本信息
中文名称 小白菊内酯
英文名称 Parthenolide
CAS号 20554-84-1
分子式 C15H20O3
分子量 248.32
EINECS号 692-532-0
InChI InChI=1S/C15H20O3/c1-9-5-4-8-15(3)13(18-15)12-11(7-6-9)10(2)14(16)17-12/h5,11-13H,2,4,6-8H2,1,3H3/b9-5+/t11-,12-,13+,15+/m0/s1
SMILES O1C(=O)C(=C)[C@]2([H])CCC(C)=CCC[C@@]3(C)O[C@]3([H])[C@@]12[H] |t:10|
物化性质
熔点 115-116 °C (lit.)
比旋光度 D20 -81.4° (c = 1.04 in chloroform); D22 -71.4° (c = 0.220 in CH2Cl2)
沸点 394.1±42.0 °C(Predicted)
密度 1.13±0.1 g/cm3(Predicted)
LogP 2.424 (est)
溶解度 可溶于DMSO(高达100mg/ml)或乙醇(高达20mg/ml)
形态 白色固体
颜色 白色
Merck 14,7048
稳定性 可在-20°下的DMSO或乙醇溶液保存长达3个月。
安全信息
危险品标志 Xi,C,F
危险类别码 11-34
安全说明 22-24/25-45-36/37/39-26-16
WGK Germany 3
RTECS号 LY4220000
海关编码 29322090
生产及用途

小白菊内酯是一种倍半萜烯内酯类天然产物,分离自艾菊、观光木等药用植物,这些植物广泛应用于发热、驱虫和抗炎等。近年来的研究证实小白菊内酯具有多种重要的药理活性,如抗肿瘤、抗病毒、抗炎和抗动脉粥样硬化等,小白菊内酯传统上主要用来治疗偏头痛、发热和类风湿性关节炎等。

倍半萜内酯类化合物小白菊内酯是从小白菊中提取的化合物,最初被用来治疗皮肤感染、风湿病以及偏头痛。近期研究表明,小白菊内酯可抑制前列腺癌、乳腺癌、胃癌、白血病癌、肾癌、肺癌、结肠腺癌、成神经管细胞瘤等癌细胞的生长,在动物模型上小白菊内酯还能治疗紫外线引起的皮肤癌。(-)-Parthenolide, Nuclear Factor-κB抑制剂,可特异性地耗尽HDAC1蛋白,而不影响其他I/II类 HDACs。促进MDM2的泛素化并激活p53的细胞功能。
TargetValue
HDAC1
NF-κB
MDM2 ubiquitination
p53
()

Parthenolide (PTL) has a dose-dependent growth inhibition effect on NSCLC cells Calu-1, H1792, A549, H1299, H157, and H460. Parthenolide can induce cleavage of apoptotic proteins such as CASP8, CASP9, CASP3 and PARP1 both in concentration- and time-dependent manner in tested lung cancer cells, indicating that apoptosis is trigged after Parthenolide exposure. In addition to induction of apoptosis, Parthenolide also induces G 0 /G 1 cell cycle arrest in a concentration-dependent manner in A549 cells and G 2 /M cell cycle arrest in H1792 cells.

Only Parthenolide, the HDAC inhibitor with anti-inflammatory features, displayed a potent anti-apoptotic effect in Phb1 KO hepatocytes. Indeed, TSA and Parthenolide-treated hepatocytes showed increased levels of FXR, and reduced levels of CYP7A1, HDAC4, TNFα, TRAIL and Bax suggesting a less toxic effect of bile acids as a results of specific HDAC inhibition, resulting in the attenuation of the Phb1 KO hepatocytes apoptotic response. Importantly, Parthenolide exerts a protective effect from the liver injury after BDL in Phb1 KO mice. Indeed, Parthenolide treatment results in a reduction of the mortality rate of this mice after BDL associated with a lower apoptotic response as revealed by a reduction of necrotic areas, Tunel-staining, as well as decreased ALT (8431±957 vs.4225±210 U/L) and AST (4805±300 vs.2242±438 U/L) activities compared to control Phb1 KO mice.

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产品供应商
20554-84-1
上海阿拉丁生化科技股份有限公司
2023-10-02

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