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通过III期黑色素瘤的分子图谱预测临床结果。

Predicting clinical outcome through molecular profiling in stage III melanoma.

作者信息

John Thomas, Black Michael A, Toro Tumi T, Leader Debbie, Gedye Craig A, Davis Ian D, Guilford Parry J, Cebon Jonathan S

机构信息

Ludwig Institute for Cancer Research, Melbourne Centre for Clinical Sciences, Austin Health, Heidelberg, Australia.

出版信息

Clin Cancer Res. 2008 Aug 15;14(16):5173-80. doi: 10.1158/1078-0432.CCR-07-4170.

Abstract

PURPOSE

Patients with macroscopic stage III melanoma represent a heterogeneous cohort with average 5-year overall survival rates of <30%. With current algorithms, it is not possible to predict which patients will achieve longer-term survival. We hypothesized that molecular profiling could be used to identify prognostic groups within patients with stage III melanoma while also providing a greater understanding of the biological programs underpinning these differences.

EXPERIMENTAL DESIGN

Lymph node sections from 29 patients with stage IIIB and IIIC melanoma, with divergent clinical outcome including 16 "poor-prognosis" and 13 "good-prognosis" patients as defined by time to tumor progression, were subjected to molecular profiling using oligonucleotide arrays as an initial training set. Twenty-one differentially expressed genes were validated using quantitative PCR and the 15 genes with strongest cross-platform correlation were used to develop two predictive scores, which were applied to two independent validation sets of 10 and 14 stage III tumor samples.

RESULTS

Supervised analysis using differentially expressed genes was able to differentiate the prognostic groups in the training set. The developed predictive scores correlated directly with clinical outcome. When the predictive scores were applied to the two independent validation sets, clinical outcome was accurately predicted in 90% and 85% of patients, respectively.

CONCLUSION

We describe a gene expression profile that is capable of distinguishing clinical outcomes in a previously homogeneous group of stage III melanoma patients.

摘要

目的

宏观分期为III期的黑色素瘤患者是一个异质性群体,其5年总生存率平均<30%。使用当前的算法,无法预测哪些患者将获得长期生存。我们假设分子谱分析可用于识别III期黑色素瘤患者中的预后组,同时还能更深入地了解造成这些差异的生物学程序。

实验设计

对29例IIIB期和IIIC期黑色素瘤患者的淋巴结切片进行分子谱分析,这些患者具有不同的临床结局,包括16例“预后不良”患者和13例“预后良好”患者(根据肿瘤进展时间定义),以此作为初始训练集。使用寡核苷酸阵列进行分子谱分析。通过定量PCR验证了21个差异表达基因,并使用具有最强跨平台相关性的15个基因开发了两个预测评分,将其应用于10例和14例III期肿瘤样本的两个独立验证集。

结果

使用差异表达基因进行的监督分析能够区分训练集中的预后组。所开发的预测评分与临床结局直接相关。当将预测评分应用于两个独立验证集时,分别在90%和85%的患者中准确预测了临床结局。

结论

我们描述了一种基因表达谱,它能够区分先前同质的III期黑色素瘤患者群体的临床结局。

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