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Failure and Success in Modern Drug Discovery: Guiding Principles in the Establishment of High Probability of Success Drug Discovery Organizations

机译:现代药物发现中的失败与成功:建立成功药物发现组织的高可能性的指导原则

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摘要

The pharmaceutical industry currently suffers unsustainably high program failure rates despite our best efforts to implement drug design methods and to develop high throughput biochemical screening technologies over the past 20 years. While much of this failure is rationalized to be due to uncontrollable late stage drug development issues and clinical events, it has become increasingly clear that the choices we make in early drug discovery are vital to the ultimate failure or success outcomes of our drug discovery programs. The judicious selection of high probability of success therapeutic modalities, the rigorous determination of leadlikeness and druglikeness, and the all-important selection of high probability of success enzyme and receptor targets are the vital drivers of failure and success in small molecule drug discovery as it is performed in the age of biochemical screening. Consideration of these guiding principles will improve our chances of success in drug discovery, and increase our ability to address unmet medical need in the future.
机译:尽管在过去20年中我们竭尽全力实施药物设计方法并开发高通量生化筛选技术,但制药行业目前仍遭受着难以维持的高程序失败率。尽管许多此类失败被合理地归因于不可控制的后期药物开发问题和临床事件,但越来越清楚的是,我们在早期药物发现中所做的选择对于我们药物发现计划的最终失败或成功结果至关重要。明智地选择成功治疗方式的高可能性,严格确定前导性和药物似性以及最重要的选择成功率高的酶和受体靶标是小分子药物发现失败和成功的关键驱动因素在生化筛选时代进行。考虑这些指导原则将增加我们在药物发现中成功的机会,并增强我们解决未满足的医疗需求的能力。

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