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221244-14-0

中文名称 4-氨基1-叔丁基-3-(1'-萘甲基)吡唑并[3,4-D]嘧啶
英文名称 1 NM-PP1
CAS 221244-14-0
分子式 C20H21N5
分子量 331.41
MOL 文件 221244-14-0.mol
更新日期 2024/05/25 01:14:12
221244-14-0 结构式 221244-14-0 结构式

基本信息

中文别名
4-氨基1-叔丁基-3-(1'-萘甲基)吡唑并[3,4-D]嘧啶
英文别名
1 NM-PP1
Chebi:52309
PP1 ANALOG II
PP1 Analog II, 1NM-PP1
MUTANT KINASES INHIBITOR II
4-AMINO-1-TERT-BUYTL-3-(1-NAPHTHYLMETHYL)PYRAZOLO[3,4-D]PYRIMIDINE
4-AMINO-1-TERT-BUTYL-3-(1'-NAPHTHYLMETHYL)PYRAZOLO[3,4-D]PYRIMIDINE
1-tert-Butyl-3-(naphthalen-1-ylmethyl)-1H-pyrazolo[3,4-D]pyrimidin-4-amine
1-(1,1-Dimethylethyl)-3-(1-naphthalenylmethyl)-1H-pyrazolo[3,4-d]pyrimidin-4-amine
所属类别
生物化工:激动剂抑制剂

物理化学性质

熔点175-176°C
沸点545.7±45.0 °C(Predicted)
密度1.25±0.1 g/cm3(Predicted)
储存条件-20°C冷冻
溶解度氯仿(微溶)、甲醇(微溶、加热)
酸度系数(pKa)4.50±0.30(Predicted)
形态白色固体
颜色白色至米色

常见问题列表

生物活性
1-NM-PP1,细胞渗透性 PP1 类似物,是一种有效的 Src 家族激酶抑制剂,对 v-Src-as1 与 c-Fyn-as1 的 IC50 值分别为 4.3 nM、3.2 nM。
靶点

IC50: 4.3 nM (v-Src-as1), 3.2 nM (c-Fyn-as1), 28 μM (v-Src), 1 μM (c-Fyn), 3.4 μM (c-Abl), 29 μM (CDK2), 24 μM (CAMKII), 120 nM (cAbl-as2), 5 nM (CDK2-as1), 8 nM (CAMKII-as1)

体外研究

Cdk7 from Cdk7 as/as or Cdk7 +/+ cells is immunoprecipitated and tested its kinase activity towards both a Pol II CTD-containing fusion protein (GST-CTD) and human Cdk2. Cdk7 recovered from the mutant, but not the wild-type, cells is inhibited by 1-NM-PP1 (1-NMPP1), with an IC 50 of ~50 nM with either substrate. Replacement of wild-type Cdk7 with Cdk7 as/as also rendered growth of HCT116 cells sensitive to 1-NM-PP1. In the absence of 1-NM-PP1, the wild-type and Cdk7 as/as cells had population doubling times of ~17.9 and ~20.2 h, respectively, with similar cell-cycle distributions in asynchronous culture, indicating minimal impairment of Cdk7 function by the F91G mutation per se. The homozygous Cdk7 as/as cells are sensitive to 1-NM-PP1, however, with an IC 50 ~100 nM measured by cell viability (MTT) assays performed after 96 h of 1-NM-PP1 exposure. In contrast, wild-type HCT116 cells are resistant to 10 μM 1-NM-PP1. Addition of 10 μM 1-NM-PP1 retards G1/S progression by the mutant but not the wild-type cells. When added simultaneously with serum to the Cdk7 as/as cells, 1-NM-PP1 prevents any progression into S phase in the next 15 h. After 24 h, there is evidence of progression into S-phase by a fraction of Cdk7 as/as cells released from serum starvation directly into medium containing 1-NM-PP1, while a fraction remained in G1. The addition of 1-NM-PP1 3 h or 6 h after serum addition delays S-phase entry by ~7 h or by ~3 h, respectively.

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