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首页> 外文期刊>Journal of Medicinal Chemistry >Discovery and Optimization of 2-Amino-4-methylquinazoline Derivatives as Highly Potent Phosphatidylinositol 3-Kinase Inhibitors for Cancer Treatment
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Discovery and Optimization of 2-Amino-4-methylquinazoline Derivatives as Highly Potent Phosphatidylinositol 3-Kinase Inhibitors for Cancer Treatment

机译:2-氨基-4-甲基喹唑啉衍生物作为高效磷脂酰肌醇3-激酶抑制剂的发现和优化用于癌症治疗

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摘要

Increased phosphatidylinositol 3-kinase (PI3K) signaling is among the most common alterations in cancer, spurring intensive efforts to develop new cancer therapeutics that target this pathway. In this work, we discovered a series of novel 2-amino-4-methylquinazoline derivatives through a hybridization and subsequent scaffold hopping approach that were highly potent class I PI3K inhibitors. Lead optimization resulted in several promising compounds (e.g., 19, 20, 37, and 43) with nanomolar PI3K potencies, prominent antiproliferative activities, favorable PK profiles, and robust in vivo antitumor efficacies. More interestingly, compared with 19 and 20, 37 and 43 demonstrated improved brain penetration and in vivo efficacy in an orthotopic glioblastoma xenograft model. Furthermore, preliminary safety assessments including hERG channel inhibition, AMES, CYP450 inhibition, and single-dose toxicity were performed to characterize their toxicological properties.
机译:增加的磷脂酰肌醇3-激酶(PI3K)信号传导是癌症中最常见的改变,促使强烈努力开发靶向该途径的新癌症治疗剂。 在这项工作中,我们通过杂交和随后的支架跳跃方法发现了一系列新的2-氨基-4-甲基喹唑啉衍生物,其是高效的I类PI3K抑制剂。 铅优化导致几种有前途的化合物(例如,19,20,37和43),具有纳摩尔PI3K疗效,突出的抗增殖活动,有利的PK型材,以及体内抗肿瘤效率的稳健。 更有趣的是,与19和20,37和43相比,在原位胶质母细胞瘤异种移植模型中表现出改善的脑渗透和体内疗效。 此外,进行初步安全评估,包括HERG通道抑制,AME,CYP450抑制和单剂量毒性,以表征其毒理学性质。

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  • 来源
    《Journal of Medicinal Chemistry》 |2018年第14期|共23页
  • 作者

    Lin Songwen; Wang Chunyang; Ji Ming; Wu Deyu; Lv Yuanhao; Zhang Kehui; Dong Yi; Jin Jing; Chen Jiajing; Zhang Jingbo; Sheng Li; Li Yan; Chen Xiaoguang; Xu Heng;

  • 作者单位

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Peking Union Med Coll Beijing 100050 Peoples R China;

    Peking Union Med Coll Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

    Chinese Acad Med Sci Inst Mat Med State Key Lab Bioact Subst &

    Funct Nat Med Beijing 100050 Peoples R China;

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  • 正文语种 eng
  • 中图分类 药学;
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