Betensky Rebecca A, Louis David N, Cairncross J Gregory
Department of Biostatistics, Harvard School of Public Health, 655 Huntington Avenue, Boston, MA 02115, USA.
J Clin Oncol. 2002 May 15;20(10):2495-9. doi: 10.1200/JCO.2002.06.140.
In solid tumor oncology, decisions regarding treatment and eligibility for trials are governed by histologic diagnosis. Despite this reliance on histology and the assumption that histology defines the disease, underlying molecular heterogeneity likely differentiates among patients' outcomes.
To illustrate how unrecognized molecular heterogeneity might obscure a truly effective new therapy for cancer, we analyzed the planning assumptions and results of a hypothetical randomized controlled trial of chemoradiotherapy for a cancer found to be drug sensitive in preliminary phase II studies.
Randomized controlled trials of effective cancer therapies can be falsely negative if therapeutic benefit is overestimated during study design because of enrichment of phase II trials for treatment-sensitive subtypes, a beneficial effect in responding patients is diluted by large numbers of nonresponding patients, or a beneficial effect in responders is reversed by a negative effect in nonresponders.
Molecular heterogeneity, if it confers different risks to patients and is unaccounted for in the design of a randomized study, can result in a clinical trial that is underpowered and fails to detect a truly effective new therapy for cancer.
在实体肿瘤肿瘤学中,关于治疗和试验资格的决策由组织学诊断决定。尽管依赖组织学且假定组织学定义疾病,但潜在的分子异质性可能导致患者预后不同。
为说明未被认识到的分子异质性如何可能掩盖一种真正有效的癌症新疗法,我们分析了一项假设的随机对照试验的规划假设和结果,该试验针对在初步II期研究中发现对药物敏感的癌症进行放化疗。
如果在研究设计期间由于II期试验中治疗敏感亚型富集而高估治疗益处、大量无反应患者稀释了反应患者的有益效果,或无反应者的负面影响逆转了反应者的有益效果,有效的癌症治疗随机对照试验可能会得出假阴性结果。
如果分子异质性给患者带来不同风险且在随机研究设计中未得到考虑,可能会导致一项临床试验效能不足,无法检测出一种真正有效的癌症新疗法。
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