The use of mechanistic biomarkers for evaluating investigational CNS compounds in early drug development.

Holly D Soares
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Abstract

Biomarkers serve as the fundamental building blocks of modern translational research strategies, and are widely implemented in current drug development. Biomarker techniques range from simple biofluid biochemical endpoints to more complex assessments, including imaging. Although biomarker usage is common throughout drug development, applications may vary depending on whether a drug candidate is in early- or late-stage testing. In early clinical drug development, biomarkers capable of providing proof of mechanism are considered critical tools in the management of attrition during phase II clinical trials. For CNS drugs, the ability to unequivocally demonstrate pharmacologically driven biological activity in the brain, as a result of the interaction of a drug with its intended target, ensures that proof-of-concept trials are designed in a manner that adequately tests the clinical efficacy hypothesis and that patients are not being exposed to inactive drugs. This review focuses on recent advances in proof-of-pharmacology biomarkers, with an emphasis on biochemical measures and simple circuit platforms used to demonstrate target engagement in central compartments.

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在早期药物开发中使用机制生物标志物来评估实验性中枢神经系统化合物。
生物标志物是现代转化研究策略的基本组成部分,在当前的药物开发中得到广泛应用。生物标志物技术的范围从简单的生物流体生化终点到更复杂的评估,包括成像。虽然生物标志物的使用在整个药物开发过程中很常见,但应用可能会因候选药物处于早期或后期测试而有所不同。在早期临床药物开发中,能够提供机制证明的生物标志物被认为是II期临床试验中管理损耗的关键工具。对于中枢神经系统药物,由于药物与预期靶点的相互作用,能够明确地证明药物在大脑中驱动的生物活性,确保概念验证试验的设计能够充分测试临床疗效假设,并且患者不会暴露于非活性药物。本文综述了最近在药理学证明生物标志物方面的进展,重点是生化测量和简单的电路平台,用于证明中央隔室的靶标参与。
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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