Oncogenes as novel targets for cancer therapy (part II): Intermediate signaling molecules.

American journal of pharmacogenomics : genomics-related research in drug development and clinical practice Pub Date : 2005-01-01 DOI:10.2165/00129785-200505040-00005

Zhuo Zhang, Mao Li, Elizabeth R Rayburn, Donald L Hill, Ruiwen Zhang, Hui Wang

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引用次数: 6

Abstract

This is the second part of a four-part review on potential therapeutic targeting of oncogenes. The previous part introduced the new technologies responsible for the advancement of oncogene identification, target validation, and drug design. Because of such advances, new specific and more efficient therapeutic agents can be developed for cancer. This part of the review continues the exploration of various oncogenes, which we have grouped within seven categories: growth factors, tyrosine kinases, intermediate signaling molecules, transcription factors, cell cycle regulators, DNA damage repair genes, and genes involved in apoptosis. Part I included a discussion of growth factors and tyrosine kinases. This portion of the review covers intermediate signaling molecules and the various strategies used to inhibit their expression or decrease their activities.

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癌基因作为癌症治疗的新靶点(第二部分):中间信号分子。

这是关于癌基因潜在治疗靶点的四部分综述的第二部分。前一部分介绍了在致癌基因鉴定、靶点验证和药物设计方面取得进展的新技术。由于这些进步，可以开发出新的特异性和更有效的治疗癌症的药物。这部分综述继续探讨各种致癌基因，我们将其分为七类:生长因子、酪氨酸激酶、中间信号分子、转录因子、细胞周期调节因子、DNA损伤修复基因和参与凋亡的基因。第一部分包括对生长因子和酪氨酸激酶的讨论。这部分综述涵盖了中间信号分子和用于抑制其表达或降低其活性的各种策略。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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American journal of pharmacogenomics : genomics-related research in drug development and clinical practice

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