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首页> 外文期刊>Journal of Medicinal Chemistry >Rational Design and Structure Validation of a Novel Peptide Inhibitor of the Adenomatous-Polyposis-Coli (APC)-Rho-Guanine-Nucleotide-Exchange-Factor-4 (Asef) Interaction
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Rational Design and Structure Validation of a Novel Peptide Inhibitor of the Adenomatous-Polyposis-Coli (APC)-Rho-Guanine-Nucleotide-Exchange-Factor-4 (Asef) Interaction

机译:腺瘤性息肉(APC)新肽抑制剂的理性设计与结构验证 - 核蝶 - 核蝶 - 核苷酸 - 晶系 - 4(ASEF)相互作用

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摘要

In colorectal cancer, adenomatous polyposis coli (APC) interacts with Rho guanine-nucleotide-exchange factor 4 (Asef), thereby stimulating aberrant colorectal-cancer-cell migration. Consequently, the APC-Asef interaction represents a promising therapeutic target for mitigating colorectal-cancer migration. In this study, we adopted the rational-design strategy involving the introduction of intramolecular hydrogen bonds and optimization of the lipophilic substituents to improve the binding affinities of peptides, leading to the discovery of MAI-400, the best inhibitor of the APC-Asef interaction known to date (K-d = 0.012 mu M, IC50 = 0.25 mu M). Comprehensive evaluation of MAI-400 by biochemical and biophysical assays revealed the formation and effect of an intramolecular hydrogen bond. A cell-based assay showed MAI-400 efficiently blocking the APC-Asef interaction in a dose-dependent manner. Therefore, our study provides a best-in-class inhibitor, MAI-400, based on the rational drug design and structural validation, that can effectively inhibit the APC-Asef interaction.
机译:在结直肠癌中,腺瘤性息肉蛋白(APC)与Rho鸟嘌呤 - 核苷酸交换因子4(ASEF)相互作用,从而刺激异常结肠直肠癌 - 细胞迁移。因此,APC-ASEF相互作用代表了用于减轻结肠直肠癌迁移的有希望的治疗靶标。在这项研究中,我们采用了涉及引入分子内氢键的理性设计策略和亲脂性取代基的优化,以改善肽的结合亲和力,导致MAI-400的发现,APC-ASEF相互作用的最佳抑制剂迄今为止已知的(KD = 0.012 mu m,IC50 =0.25μm)。通过生化和生物物理测定对MAI-400的综合评价显示了分子内氢键的形成和效果。基于细胞的测定显示MAI-400以剂量依赖性方式有效地阻断APC-ASEF相互作用。因此,我们的研究提供了一流的抑制剂MAI-400,基于合理的药物设计和结构验证,可以有效地抑制APC-ASEF相互作用。

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  • 来源
    《Journal of Medicinal Chemistry》 |2018年第17期|共12页
  • 作者

    Yang Xiuyan; Zhong Jie; Zhang Qinfen; Qian Jinxing; Song Kun; Ruan Cong; Xu Jianrong; Ding Ke; Zhang Jian;

  • 作者单位

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Dept Pharmacol Inst Med Sci Shanghai 200025 Peoples R China;

    Jinan Univ Sch Pharm 601 Huangpu Ave West Guangzhou 510632 Guangdong Peoples R China;

    Shanghai Jiao Tong Univ Sch Med Chinese Minist Educ Dept Pathophysiol Key Lab Cell Differentiat &

    Apo Shanghai 200025 Peoples R China;

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  • 正文语种 eng
  • 中图分类 药学;
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