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首页> 外文期刊>Seminars in cancer biology >Emergence and prevention of resistance against small molecule inhibitors.
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Emergence and prevention of resistance against small molecule inhibitors.

机译:对小分子抑制剂的出现和预防。

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Small molecule inhibitors target specific metabolic pathways in tumor cells and are a promising class of drugs for the treatment of cancers. The best known example is the treatment of chronic myeloid leukemia (CML) with Gleevec. This is a small molecule inhibitor of the Bcr-Abl kinase which has been shown to drive the initiation and progression of CML. While treatment of early stage CML with Gleevec has been quite successful, later stages of the disease (blast crisis) are not successfully treated due to the emergence of drug resistant cells. It is therefore important to understand the principles according to which drug resistant cells evolve, so that we can design treatment strategies which aim to prevent the rise of resistant cells. Such evolutionary dynamics can be studied with mathematical models, and this article reviews such an approach. We address three specific questions: (i) Do resistant cells emerge before or after the start of therapy? (ii) How does the turnover rate of cancer cells influencethe evolution of drug resistant cells? (iii) Can combination therapy be used to prevent drug resistance? We apply our model to the treatment of CML with Gleevec, in order to demonstrate how this mathematical framework can be applied to the treatment of a specific cancer with small molecule inhibitors.
机译:小分子抑制剂靶向肿瘤细胞中特定的代谢途径,是治疗癌症的有前途的一类药物。最著名的例子是格列卫治疗慢性粒细胞白血病(CML)。这是Bcr-Abl激酶的小分子抑制剂,已显示出它能驱动CML的发生和发展。用格列卫治疗早期CML已相当成功,但由于耐药细胞的出现,未能成功治疗疾病的晚期(疾风危机)。因此,重要的是要理解耐药细胞进化所依据的原理,以便我们可以设计旨在防止耐药细胞升高的治疗策略。可以使用数学模型研究这种进化动力学,本文将对这种方法进行综述。我们解决三个具体问题:(i)在治疗开始之前或之后会出现耐药细胞吗? (ii)癌细胞的周转率如何影响耐药细胞的进化? (iii)可以采用联合疗法预防耐药性吗?我们将我们的模型应用于格列卫治疗CML,以证明该数学框架如何应用小分子抑制剂治疗特定癌症。

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