在抗癌药物早期临床试验中进行序贯肿瘤活检以进行药效学评估。

Sequential tumor biopsies in early phase clinical trials of anticancer agents for pharmacodynamic evaluation.

作者信息

Dowlati A, Haaga J, Remick S C, Spiro T P, Gerson S L, Liu L, Berger S J, Berger N A, Willson J K

机构信息

Division of Hematology/Oncology, Department of Medicine, Ireland Cancer Center at University Hospitals of Cleveland, 11100 Euclid Avenue, Cleveland, OH 44106, USA.

出版信息

Clin Cancer Res. 2001 Oct;7(10):2971-6.

PMID:11595684

Abstract

PURPOSE

In the setting of target-based anticancer drug development, it is critical to establish that the observed preclinical activity can be attributed to modulation of the intended target in early phase trials in human subjects. This paradigm of target modulation allows us to determine a Phase II or III dose (optimal biochemical/biological modulatory dose) that may not necessarily be the maximum tolerated dose. A major obstacle to target-based (often cytostatic) drug development has been obtaining relevant tumor tissue during clinical trials of these novel agents for laboratory analysis of the putative marker of drug effect.

EXPERIMENTAL DESIGN

From 1989 to present, we have completed seven clinical trials in which the end point was a biochemical or biological modulatory dose in human tumor tissues (not surrogate tissue). Eligibility enrollment required that patients have a biopsiable lesion either with computerized tomography (CT) guidance or direct visualization and consent to sequential (pre and posttreatment) biopsies.

RESULTS

A total of 192 biopsies were performed in 107 patients. All but 8 patients had sequential pre and posttreatment biopsies. Seventy-eight (73%) of the 107 patients had liver lesion biopsies. In eight patients, either one or both biopsies contained insufficient viable tumor tissue or no tumor tissue at all for analysis. Of a total of 99 patients in whom we attempted to obtain paired biopsies, a total of 87 (88%) were successful. Reasons for failure included patient refusal for a second biopsy (n = 2), vasovagal reaction with first biopsy precluding a second biopsy (n = 1), subcapsular hepatic bleeding (n = 1), and most commonly obtaining necrotic tumor, fibrous, or normal tissue in one of the two sequential biopsies (n = 8).

CONCLUSIONS

This is the first and largest reported series demonstrating that with adequate precautions and experience, sequential tumor biopsies are feasible and safe during early phase clinical trials.

摘要

目的

在基于靶点的抗癌药物研发背景下，至关重要的是要证实观察到的临床前活性可归因于人体早期试验中对预期靶点的调节。这种靶点调节模式使我们能够确定可能不一定是最大耐受剂量的II期或III期剂量（最佳生化/生物调节剂量）。基于靶点（通常为细胞生长抑制剂）的药物研发的一个主要障碍是在这些新型药物的临床试验期间获取相关肿瘤组织用于药物效应假定标志物的实验室分析。

实验设计

从1989年至今，我们完成了7项临床试验，其终点是人体肿瘤组织（而非替代组织）中的生化或生物调节剂量。入选标准要求患者在计算机断层扫描（CT）引导下或直接可视化下有可活检的病变，并同意进行序贯（治疗前和治疗后）活检。

结果

对107例患者共进行了192次活检。除8例患者外，所有患者均进行了序贯的治疗前和治疗后活检。107例患者中有78例（73%）进行了肝脏病变活检。8例患者的一次或两次活检所获活肿瘤组织不足或根本没有肿瘤组织可供分析。在我们试图获取配对活检的99例患者中，共有87例（88%）成功。失败原因包括患者拒绝进行第二次活检（n = 2）、首次活检时出现血管迷走神经反应导致无法进行第二次活检（n = 1）、肝包膜下出血（n = 1），最常见的是在两次序贯活检中的一次获取到坏死肿瘤、纤维组织或正常组织（n = 8）。