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多发性骨髓瘤完全缓解的益处仅限于通过基因表达谱鉴定的高危亚组。

Benefit of complete response in multiple myeloma limited to high-risk subgroup identified by gene expression profiling.

作者信息

Haessler Jeffrey, Shaughnessy John D, Zhan Fenghuang, Crowley John, Epstein Joshua, van Rhee Frits, Anaissie Elias, Pineda-Roman Mauricio, Zangari Maurizio, Hollmig Klaus, Mohiuddin Abid, Alsayed Yazan, Hoering Antje, Tricot Guido, Barlogie Bart

机构信息

Cancer Research and Biostatistics, Seattle, Washington, USA.

出版信息

Clin Cancer Res. 2007 Dec 1;13(23):7073-9. doi: 10.1158/1078-0432.CCR-07-0527.

Abstract

EXPERIMENTAL DESIGN

To determine whether the clinical benefit of complete remission (CR) may depend on prognostic subgroups of patients with multiple myeloma.

PATIENTS AND METHODS

Newly diagnosed patients with myeloma received a tandem autotransplant regimen. Using multivariate regression analyses, we examined the prognostic implications of time-dependent onset of CR on overall survival and event-free survival in the context of standard prognostic factors (SPF) and gene expression profiling-derived data available for 326 patients.

RESULTS

CR benefited patients regardless of risk status when only SPFs were examined. With knowledge of gene array data, a survival (and event-free survival) benefit of CR only pertained to the small high-risk subgroup of 13% of patients (hazard ratio, 0.23; P = 0.001), whereas the majority of patients with low-risk disease had similar survival expectations whether or not CR was achieved (hazard ratio, 0.68; P = 0.128).

CONCLUSIONS

Access to gene expression information permitted the recognition of a small very high-risk subgroup of 13% of patients, in whom prolonged survival critically depended on achieving CR. Absence of such benefit in the remainder should lead to a reassessment of clinical trial designs that rely on this end point as a surrogate for long-term prognosis.

摘要

实验设计

确定完全缓解(CR)的临床益处是否可能取决于多发性骨髓瘤患者的预后亚组。

患者与方法

新诊断的骨髓瘤患者接受串联自体移植方案。我们使用多变量回归分析,在326例患者可获得的标准预后因素(SPF)和基因表达谱数据的背景下,研究CR的时间依赖性发生对总生存期和无事件生存期的预后影响。

结果

仅检查SPF时,无论风险状态如何,CR对患者均有益。了解基因阵列数据后,CR的生存(和无事件生存)益处仅适用于13%的小高危亚组患者(风险比,0.23;P = 0.001),而大多数低风险疾病患者无论是否实现CR,其生存预期相似(风险比,0.68;P = 0.128)。

结论

获取基因表达信息使得能够识别出13%的小极高危亚组患者,这些患者的长期生存严重依赖于实现CR。其余患者缺乏这种益处应促使重新评估依赖这一终点作为长期预后替代指标的临床试验设计。

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