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SML0778

Sigma-Aldrich

UNC1999

≥98% (HPLC)

别名:

1-Isopropyl-6-(6-(4-isopropylpiperazin-1-yl)pyridin-3-yl)-N-((6-methyl-2-oxo-4-propyl-1,2-dihydropyridin-3-yl)methyl)-1H-indazole-4-carboxamide

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About This Item

经验公式(希尔记法):
C33H43N7O2
CAS号:
1431612-23-5
分子量:
569.74
MDL编号:
MFCD26960958
UNSPSC代码:
41121800
PubChem化学物质编号:
329825598
NACRES:
NA.77

质量水平

100

方案

≥98% (HPLC)

表单

powder

颜色

white to beige

溶解性

DMSO: 15 mg/mL, clear

储存温度

2-8°C

SMILES字符串

CC(C)N1CCN(C2=NC=C(C3=CC4=C(C=NN4C(C)C)C(C(NCC5=C(CCC)C=C(C)NC5=O)=O)=C3)C=C2)CC1

InChI

1S/C33H43N7O2/c1-7-8-24-15-23(6)37-33(42)28(24)19-35-32(41)27-16-26(17-30-29(27)20-36-40(30)22(4)5)25-9-10-31(34-18-25)39-13-11-38(12-14-39)21(2)3/h9-10,15-18,20-22H,7-8,11-14,19H2,1-6H3,(H,35,41)(H,37,42)

InChI key

DPJNKUOXBZSZAI-UHFFFAOYSA-N

相关类别

生化/生理作用

UNC1999 是 EZH2 和 EZH1 赖氨酸甲基转移酶的口服生物可利用选择性抑制剂。
多梳抑制络合物 2 (PRC2)通过组蛋白 H3 在赖氨酸 27 (H3K27) 上的甲基化来抑制基因表达,其中包含作为其的催化亚基的EZH1 或 EZH2 ,EZH1 在分裂细胞和非分裂细胞中均有发现,而 EZH2 仅在活跃分裂细胞中有发现。UNC1999 是一种口服的 EZH2 和 EZH1 赖氨酸甲基转移酶的选择性抑制剂,同时IC 50 < 10 nM (EZH2)和 IC 50< 45 nM (EZH1)。UNC1999 强效抑制野生型和突变型 Y641N EZH2 甲基转移酶活性的能力相差不到 5 倍,并选择性杀死携带 Y641 点突变的弥散性大 B 细胞淋巴瘤(DLBCL)细胞。它对 EZH2 和 EZH1 的选择性高于其他 15 种赖氨酸、精氨酸和 DNA 甲基转移酶。UNC1999 与辅因子 S-腺苷甲硫氨酸(SAM)竞争,但不与肽底物竞争。因为它同时抑制 EZH2 和 EZH1,在 PRC2–EZH2 和 PRC2–EZH1 都促进 H3K27 甲基化的疾病环境中,UNC1999 比 EZH2 选择性抑制剂有潜在的优势。

有关表征的完整详细信息,请访问结构基因组学联盟(SGC)网站上的 UNC1999 探针摘要

UNC2400 是活性探针 UNC1999 的阴性对照物。要从SGC 获取阴性对照样品, 单击此处

想要了解用于表观遗传靶标的其他SGC化学探针,请访问sigma.com/sgc

特点和优势

UNC1999是一种表观遗传化学探针,是我们与Structural Genomics Consortium (SGC) 合作研发的。想要了解更多信息并查看其他SGC表观遗传探针,请访问sigma.com/SGC
这种化合物是基因调控研究的特色产物。点击此处查看更多特色基因调控产物。登录sigma.com/discover-bsm可了解更多关于其他研究领域中关于生物活性小分子的消息。

其他说明

在化学探针门户网站上,已有专家审查和推荐了UNC1999。欲了解更多信息,请访问化学探针门户网站上的 UNC1999 探针摘要

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储存分类代码

11 - Combustible Solids

WGK

WGK 3

闪点(°F)

Not applicable

闪点(°C)

Not applicable

历史批次信息供参考:

分析证书(COA)

Lot/Batch Number
0000242233
0000239521
0000239523
0000235684
0000239521

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Peter E Feist et al.
Analytical chemistry, 89(5), 2773-2781 (2017-02-15)
Multicellular tumor spheroids (MCTS) are valuable in vitro tumor models frequently used to evaluate the penetration and efficacy of therapeutics. In this study, we evaluated potential differences in epigenetic markers, i.e., histone post-translational modifications (PTMs), in the layers of the
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Epigenetics & chromatin, 11(1), 23-23 (2018-05-29)
MMP-9 plays a direct role in the activation of pro-osteoclastogenic genes by cleaving histone H3N-terminal tail (H3NT) and altering chromatin architecture. Although H3 acetylation at K18 has been shown to stimulate MMP-9 enzymatic activity toward H3NT, nothing is known about
Chen Hou et al.
Frontiers in genetics, 13, 1013475-1013475 (2022-10-25)
Although gene mutations and aberrant chromosomes are associated with the pathogenesis and prognosis of uveal melanoma (UM), potential therapeutic targets still need to be explored. We aim to determine the predictive value and potential therapeutic target of EZH2 in uveal
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Cancer discovery, 10(9), 1312-1329 (2020-06-18)
Tumor progression upon treatment arises from preexisting resistant cancer cells and/or adaptation of persister cancer cells committing to an expansion phase. Here, we show that evasion from viral mimicry response allows the growth of taxane-resistant triple-negative breast cancer (TNBC). This
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