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伴随诊断试剂的可及性对抗癌药物临床开发的影响

Impact of Availability of Companion Diagnostics on the Clinical Development of Anticancer Drugs.

作者信息

Tibau Ariadna, Díez-González Laura, Navarro Beatriz, Galán-Moya Eva M, Templeton Arnoud J, Seruga Bostjan, Pandiella Atanasio, Amir Eitan, Ocana Alberto

机构信息

Hospital Santa Crau y Sant Pau, Barcelona, Spain.

Translational Research Unit, CIBERONC, Albacete University Hospital, Albacete, Spain.

出版信息

Mol Diagn Ther. 2017 Jun;21(3):337-343. doi: 10.1007/s40291-017-0267-y.

DOI:10.1007/s40291-017-0267-y
PMID:28247182
Abstract

BACKGROUND

Companion diagnostics permit the selection of patients likely to respond to targeted anticancer drugs; however, it is unclear if the drug development process differs between drugs developed with or without companion diagnostics. Identification of differences in study design could help future clinical development.

PATIENTS AND METHODS

Anticancer drugs approved for use in solid tumors between 28 September 2000 and 4 January 2014 were identified using a search of the US FDA website. Phase III trials supporting registration were extracted from the drug label. Each published study was reviewed to obtain information about the phase I and II trials used for the development of the respective drug.

RESULTS

We identified 35 drugs and 59 phase III randomized trials supporting regulatory approval. Fifty-three phase I trials and 47 phase II trials were cited in the studies and were used to support the design of these phase III trials. The approval of drugs using a companion diagnostic has increased over time (p for trend 0.01). Expansion cohorts were more frequently observed with drugs developed with a companion diagnostic (62 vs. 20%; p = 0.005). No differences between drugs developed with or without a companion diagnostic were observed for the design of phase I and II studies.

CONCLUSIONS

The approval of drugs developed with a companion diagnostic has increased over time. The availability of a companion diagnostic was associated with more frequent use of phase I expansion cohorts comprising patients selected by the companion diagnostic.

摘要

背景

伴随诊断有助于筛选可能对靶向抗癌药物产生反应的患者;然而,尚不清楚使用或不使用伴随诊断开发的药物,其研发过程是否存在差异。识别研究设计中的差异有助于未来的临床开发。

患者和方法

通过搜索美国食品药品监督管理局(US FDA)网站,确定2000年9月28日至2014年1月4日期间批准用于实体瘤的抗癌药物。从药物标签中提取支持注册的III期试验。对每项已发表的研究进行审查,以获取有关用于各自药物开发的I期和II期试验的信息。

结果

我们确定了35种药物和59项支持监管批准的III期随机试验。研究中引用了53项I期试验和47项II期试验,并用于支持这些III期试验的设计。使用伴随诊断的药物批准率随时间增加(趋势p值为0.01)。在使用伴随诊断开发的药物中,更频繁地观察到扩展队列(62%对20%;p = 0.005)。在I期和II期研究设计中,未观察到使用或不使用伴随诊断开发的药物之间存在差异。

结论

使用伴随诊断开发的药物批准率随时间增加。伴随诊断的可用性与更频繁地使用由伴随诊断选择的患者组成的I期扩展队列相关。

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