Using mouse forward genetics to define novel target space

Nancy A. Hong, Steve A. Kay, Richard J. Glynne
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引用次数: 1

Abstract

Rapid advances in genomics technologies have identified a wealth of new therapeutic targets, but typically these targets are weakly validated with only circumstantial evidence to link them to human disease. The next challenge is testing gene-to-disease connections in a relevant animal model, a time-consuming and uncertain process using conventional reverse-genetic approaches such as knockout and transgenic mice. By contrast, forward genetics proceeds by measuring a physiological process that is relevant to disease, then identifying the gene products that impinge on this process. This ‘phenotype-first’ approach solves the bottleneck of target validation by using clinically relevant assays in a mammalian whole-animal system as a discovery platform. As an unbiased approach to gene discovery and validation, forward genetics will identify novel drug targets and increase the success rate of drug development.

利用小鼠前向遗传学定义新的目标空间
基因组学技术的快速发展已经确定了大量新的治疗靶点,但通常这些靶点的有效性很弱,只有间接证据将它们与人类疾病联系起来。下一个挑战是在相关的动物模型中测试基因与疾病的联系,这是一个耗时且不确定的过程,使用传统的反遗传方法,如基因敲除和转基因小鼠。相比之下,正向遗传学通过测量与疾病相关的生理过程,然后识别影响这一过程的基因产物来进行。这种“表型优先”的方法通过在哺乳动物全动物系统中使用临床相关分析作为发现平台,解决了靶标验证的瓶颈。作为一种公正的基因发现和验证方法,正向遗传学将识别新的药物靶点,提高药物开发的成功率。
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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