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变劣势为优势:基于非靶标药物的癌症再利用。

Turning liabilities into opportunities: Off-target based drug repurposing in cancer.

机构信息

Department of Drug Discovery, H. Lee Moffitt Cancer Center & Research Institute, Tampa, FL, 33612, USA.

Department of Drug Discovery, H. Lee Moffitt Cancer Center & Research Institute, Tampa, FL, 33612, USA.

出版信息

Semin Cancer Biol. 2021 Jan;68:209-229. doi: 10.1016/j.semcancer.2020.02.003. Epub 2020 Feb 7.

Abstract

Targeted drugs and precision medicine have transformed the landscape of cancer therapy and significantly improved patient outcomes in many cases. However, as therapies are becoming more and more tailored to smaller patient populations and acquired resistance is limiting the duration of clinical responses, there is an ever increasing demand for new drugs, which is not easily met considering steadily rising drug attrition rates and development costs. Considering these challenges drug repurposing is an attractive complementary approach to traditional drug discovery that can satisfy some of these needs. This is facilitated by the fact that most targeted drugs, despite their implicit connotation, are not singularly specific, but rather display a wide spectrum of target selectivity. Importantly, some of the unintended drug "off-targets" are known anticancer targets in their own right. Others are becoming recognized as such in the process of elucidating off-target mechanisms that in fact are responsible for a drug's anticancer activity, thereby revealing potentially new cancer vulnerabilities. Harnessing such beneficial off-target effects can therefore lead to novel and promising precision medicine approaches. Here, we will discuss experimental and computational methods that are employed to specifically develop single target and network-based off-target repurposing strategies, for instance with drug combinations or polypharmacology drugs. By illustrating concrete examples that have led to clinical translation we will furthermore examine the various scientific and non-scientific factors that cumulatively determine the success of these efforts and thus can inform the future development of new and potentially lifesaving off-target based drug repurposing strategies for cancers that constitute important unmet medical needs.

摘要

靶向药物和精准医学改变了癌症治疗的格局,在许多情况下显著改善了患者的预后。然而,随着治疗方法越来越针对较小的患者群体,并且获得性耐药性限制了临床反应的持续时间,对新药的需求不断增加,考虑到药物淘汰率和开发成本的稳步上升,这一需求并不容易满足。考虑到这些挑战,药物再利用是一种有吸引力的、与传统药物发现互补的方法,可以满足其中的一些需求。这是因为大多数靶向药物,尽管它们有隐含的含义,但并不是单一的特异性,而是显示出广泛的靶标选择性。重要的是,一些意外的药物“非靶标”本身就是已知的抗癌靶点。其他的则在阐明非靶标机制的过程中被认为是这样的,而这些机制实际上负责药物的抗癌活性,从而揭示了潜在的新的癌症脆弱性。因此,利用这些有益的非靶标效应可以导致新的、有前途的精准医学方法。在这里,我们将讨论用于专门开发单靶标和基于网络的非靶标再利用策略的实验和计算方法,例如药物组合或多药理学药物。通过举例说明导致临床转化的具体例子,我们将进一步研究决定这些努力成功的各种科学和非科学因素,从而为构成重要未满足医疗需求的癌症提供基于新的、潜在的挽救生命的非靶标药物再利用策略的未来发展提供信息。

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