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Selective Actionable and Druggable Protein Kinases Drive the Progression of Neuroendocrine Prostate Cancer

机译:选择性可操作和可药栓蛋白激酶驱动神经内分泌前列腺癌的进展

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摘要

Current clinical anti-androgen therapies in advanced prostate cancer (PCa) are driving an increased incidence of neuroendocrine prostate cancer (NEPC), a histological variant exhibiting reduced androgen receptor levels and expression of neuroendocrine markers. The mechanisms underlying the development of NEPC are poorly understood. A set of available data from a well-validated xenograft model of NEPC was used to analyze the exact role of protein kinase (PK) played in the development of NEPC. Fifty-four actionable and druggable PKs, mainly enriched in PI3K-Akt, mTOR, and MAPK signaling pathways, were screened out from the drastically changed PKs during NEPC transdifferentiation. Further analysis based on the crosstalk of these above signaling pathways finally singled out 10 PKs considered drivers and therapeutic targets in the development and treatment of NEPC. In vitro, the variation trend of PK expression observed during NEPC transdifferentiation could be recapitulated in PCa cell lines with different malignant degree. The predicted kinase targets exhibited different sensibilities in the restriction of PC3 cell growth. Selective actionable and druggable PKs may act as drivers in the progression of NEPC, and most of them can be used as potential therapeutic targets in clinical practice.
机译:目前晚期前列腺癌(PCA)的临床抗雄激素疗法正在推动神经内分泌前列腺癌(NEPC)的发病率增加,其组织学变体表现出降低的雄激素受体水平和神经内分泌标记的表达。核心发展的机制理解得很差。来自核心良好验证的Xenograff模型的一组可用数据用于分析蛋白激酶(PK)在Nepc发育中起作用的确切作用。在NEPC转置异化期间,从巨大改变的PKS筛选出在PI3K-AKT,MTOR和MAPK信号传导途径中富集的五十四个可致力于富集的PKS。基于上述信号通路的串扰的进一步分析最终挑出了10个PKS考虑了Nepc的发育和治疗中的司机和治疗目标。体外,在具有不同恶性程度的PCA细胞系中,可以重新观察到在NepC转染术期间观察到的PK表达的变化趋势。预测的激酶靶标在PC3细胞生长的限制中表现出不同的敏感性。选择性可操作和可药剂的PKS可以作为奈培进展的司机,并且大多数可以用作临床实践中的潜在治疗目标。

著录项

  • 来源
    《DNA and Cell Biology》 |2018年第9期|共9页
  • 作者单位

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Dept Urol Sino Singapore Ecocity Hosp Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

    Tianjin Med Univ Hosp 2 Dept Urol Tianjin Inst Urol Tianjin Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞遗传学;
  • 关键词

    neuroendocrine prostate cancer; protein kinase; bioinformatics analysis; targeted therapy;

    机译:神经内分泌前列腺癌;蛋白激酶;生物信息学分析;有针对性的治疗;

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