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SCR7 pyrazine

CAS号

14892-97-8

分子式

C18H12N4OS

主要靶点

Apoptosis|CRISPR/Cas9|DNA/RNA Synthesis

仅限科研使用

Cat No : CM03745

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Synonyms

end-joining|DNASynthesis|DNA Synthesis|DNALigase IV|DNA/RNA Synthesis|CRISPR|CRISPR/Cas9|Apoptosis|Cas9|Caspase 3|Caspase 9|SCR-7|SCR7 pyrazine|SCR-7 pyrazine|SCR7 吡嗪|SCR 7|ligase-IV|replacement|RNASynthesis|RNA Synthesis|nonhomologous

验证数据展示

  • CAS No.: 14892-97-8

    SCR7 pyrazine
    CAS#: 14892-97-8

产品信息

CAS号 14892-97-8
分子式 C18H12N4OS
主要靶点 Apoptosis|CRISPR/Cas9|DNA/RNA Synthesis
主要通路 DNA 损伤和修复|细胞周期|DNA 损伤和修复|凋亡
分子量 332.38
纯度 99.85%, 此纯度可做参考,具体纯度与批次有关系,可咨询客服
储存条件 Powder: -20°C for 3 years | In solvent: -80°C for 1 year | Shipping with blue ice.
别名 end-joining|DNASynthesis|DNA Synthesis|DNALigase IV|DNA/RNA Synthesis|CRISPR|CRISPR/Cas9|Apoptosis|Cas9|Caspase 3|Caspase 9|SCR-7|SCR7 pyrazine|SCR-7 pyrazine|SCR7 吡嗪|SCR 7|ligase-IV|replacement|RNASynthesis|RNA Synthesis|nonhomologous

体内活性

SCR7处理(10 mg/kg,肌肉注射)显著减少了乳腺腺癌诱导的肿瘤,并且与对照组相比,生命期增加了4倍。然而,在携带Dalton's淋巴瘤肿瘤模型的瑞士白鼠中,SCR7(20 mg/kg,腹腔注射)既不表现出肿瘤退缩也不增加生命期。在BALB/c小鼠中,SCR7(20 mg/kg,腹腔注射)显著增强了辐射、依托泊苷和3-氨基苯甲酰胺对源自Dalton's淋巴瘤(DLA)细胞的肿瘤的细胞毒作用。[1]

体外活性

SCR7在200μM及以上浓度下有效抑制多聚体的形成。SCR7成功抑制了MCF7、A549、HeLa、T47D、A2780、HT1080和Nalm6细胞的增殖,其IC50分别为40、34、44、8.5、120、10和50μM。[1] SCR7抑制了CRISPR-Cas9诱导的DSBs的NHEJ修复。[2]

溶解度

DMSO:66 mg/mL (198.57 mM);H2O:< 1 mg/mL (insoluble or slightly soluble);Ethanol:3 mg/mL (9.03 mM)

细胞实验

Cell proliferation of cancer cells are determined by MTT and trypan blue assays. Briefly, MCF7, CEM, HeLa, A549, HT1080, A2780, T47D, Nalm6, N114 and K562 cells are grown in presence of SCR7 (10, 50, 100, and 250?μM) for 24 or 48?h, and subjected to MTT or trypan blue assays. Each experiment is repeated a minimum of three independent times. (Only for Reference)

参考文献

1.Srivastava M, et al. Cell. 2012, 151(7), 1474-1487.
2.Chu VT, et al. Nat Biotechnol. 2015, doi: 10.1038/nbt.3198.

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Concentration (start) × Volume (start) = Concentration (final) × Volume (final)
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