Phase 0 clinical trials: theoretical and practical implications in oncologic drug development

IF 1.4 Q4 MEDICINE, RESEARCH & EXPERIMENTAL

Open Access Journal of Clinical Trials Pub Date : 2013-10-01 DOI:10.2147/OAJCT.S32978

P. Coloma

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引用次数: 6

Abstract

textabstractDrug discovery and development has become a risky, expensive, and protracted process, with the cost of introducing a new drug to the market going as high as US$2 billion and the entire process taking at least 10-15 years. Great advances in biomedical research in recent years have not resulted in translation into medical product development, and there has been substantial decline in both new drug applications and biological license applications. To address this so-called "pipeline problem," both the US Food and Drug Administration and its European counterpart, the European Agency for the Evaluation of Medicinal Products (now European Medicines Agency) endorsed the concept of Phase 0 studies (also known as exploratory investigational new drug studies), aimed towards identifying, early in the process of drug development, viable candidates and eliminating those lacking promise. Primary study endpoints of trials conducted under an exploratory investigational new drug can include evaluation of analogs for lead selection, modulation of a molecular target in vivo, whole-body imaging for tissue distribution/target binding affinity, and agent pharmacokinetics. Phase 0 trials bridge the gap between traditional preclinical testing and clinical studies and are intended to provide a better understanding of a new compound's pharmacokinetics, pharmacodynamics, and target localization before initiation of Phase I trials. When such information can be obtained earlier, decisions regarding drug development can also be made at an earlier point in time, potentially reducing costs of initial preclinical studies and time-to-first-in-human testing. This review provides an overview of the various conditions that have to be met in order for a Phase 0 trial to be successful, citing examples of two candidate drugs that have been further developed after Phase 0 trials in oncology. Challenges and opportunities with Phase 0 trials are discussed, including ethical issues associated with trials that have no therapeutic or diagnostic intent.

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0期临床试验:肿瘤药物开发的理论和实践意义

药物发现和开发已经成为一个高风险、昂贵和旷日持久的过程，将一种新药推向市场的成本高达20亿美元，整个过程至少需要10-15年。近年来，生物医学研究取得的巨大进展并未转化为医疗产品开发，新药申请和生物许可证申请均大幅下降。为了解决这个所谓的“管道问题”，美国食品和药物管理局及其欧洲同行，欧洲药品评估局(现为欧洲药品管理局)都认可了0期研究的概念(也称为探索性研究新药研究)，旨在在药物开发过程的早期确定可行的候选药物并消除那些缺乏希望的药物。在探索性研究新药下进行的试验的主要研究终点可以包括对铅选择的类似物的评估，体内分子靶点的调节，组织分布/靶点结合亲和力的全身成像，以及药物的药代动力学。0期试验弥补了传统临床前试验和临床研究之间的差距，旨在在I期试验开始前更好地了解新化合物的药代动力学、药效动力学和靶点定位。如果能够更早地获得此类信息，就可以在更早的时间点做出有关药物开发的决定，从而可能降低初步临床前研究的成本和首次人体试验的时间。本综述概述了成功的0期临床试验必须满足的各种条件，并引用了两种候选药物的例子，这两种候选药物在肿瘤0期临床试验后得到了进一步的开发。讨论了0期试验的挑战和机遇，包括与无治疗或诊断意图的试验相关的伦理问题。

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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来源期刊

Open Access Journal of Clinical Trials MEDICINE, RESEARCH & EXPERIMENTAL-

CiteScore

3.90

自引率

0.00%

发文量

审稿时长

16 weeks