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    首页 分子通 7,9-Dimethyl-2,6-bis-(methylthio)purin-8-thion

    7,9-Dimethyl-2,6-bis-(methylthio)purin-8-thion | 51292-19-4

    分子结构分类

    有机化合物 - 有机杂环化合物 - 咪唑并嘧啶类
    中文名称
    ——
    中文别名
    ——
    英文名称
    7,9-Dimethyl-2,6-bis-(methylthio)purin-8-thion
    英文别名
    7,9-dimethyl-2,6-bis-methylsulfanyl-7,9-dihydro-purine-8-thione
    7,9-Dimethyl-2,6-bis-(methylthio)purin-8-thion化学式
    CAS
    51292-19-4
    化学式
    C9H12N4S3
    mdl
    ——
    分子量
    272.419
    InChiKey
    NBCOZZZHIUNSQV-UHFFFAOYSA-N
    BEILSTEIN
    ——
    EINECS
    ——
    • 物化性质
    • 计算性质
    • ADMET
    • 安全信息
    • SDS
    • 制备方法与用途
    • 上下游信息
    • 反应信息
    • 文献信息
    • 表征谱图
    • 同类化合物
    • 相关功能分类
    • 相关结构分类

    反应信息

    • 作为产物:
      描述:
      碘甲烷7,9-二氢-3H-嘌呤-2,6,8-三硫酮1,8-二氮杂双环[5.4.0]十一碳-7-烯 作用下, 以 N,N-二甲基甲酰胺 为溶剂, 反应 0.08h, 以17%的产率得到9-methyl-2,6-bis(methylthio)-7,9-dihydro-8H-purine-8-thione
      参考文献:
      名称:
      The discovery of purine-based agents targeting triple-negative breast cancer and the αB-crystallin/VEGF protein–protein interaction
      摘要:
      Oestrogen receptor-negative breast cancer, particularly subtypes such as triple-negative breast cancer (TNBC, around 10-15% of cases), are characterised by poor long-term survival, poor response to therapy and early progression to metastasis. Purine-based compounds represent a privileged scaffold in anticancer drug design, with several clinically approved and experimental agents in clinical development comprising a purine core structure. In this study, a series of new purine-based compounds were synthesised; seven of the new analogues were found to significantly reduce the in vitro viability of TNBC cell lines (MDA-MB-231 and MDA-MB-436) with IC50 values of 50M. In previous work, we have proposed a new concept for targeting angiogenesis driving TNBC progression, by disrupting the protein-protein interaction between the molecular chaperone B-crystallin (CRYAB) and VEGF. Since previous clinical studies applying anti-VEGF therapy to TNBC patients have met with limited success, we were interested to test our most promising purine analogues against CRYAB/VEGF, using a custom-designed cell-based CRYAB/VEGF(165) interaction assay platform. Analogues 4e and 4f significantly reduced the interaction between CRYAB/VEGF(165), and compound 4e (100M) was also found to decrease the levels of soluble VEGF expressed by MDA-MB-231 cells by 40%. In conclusion, these promising early activity profiles warrant further investigation to validate this concept.
      DOI:
      10.1007/s00044-018-2275-9
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