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年轻女性和黑人女性乳腺癌中 21 基因和 PAM50 复发评分的差异。

Differences in 21-Gene and PAM50 Recurrence Scores in Younger and Black Women With Breast Cancer.

机构信息

Lineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC.

Department of Epidemiology, Gillings School of Public Health, University of North Carolina at Chapel Hill, Chapel Hill, NC.

出版信息

JCO Precis Oncol. 2024 Jul;8:e2400137. doi: 10.1200/PO.24.00137.

Abstract

PURPOSE

Genomic tests, such as the Oncotype Dx 21-gene and Prosigna risk of recurrence (ROR-P) assay, are commonly used for breast cancer prognostication. Emerging data suggest variability between assays, but this has not been compared in diverse populations.

MATERIALS AND METHODS

RNA sequencing was performed on 647 previously untreated stage I-III estrogen receptor-positive/human epidermal growth factor receptor 2-negative tumors in the Carolina Breast Cancer Study, which oversampled Black and younger women (age <50 years at diagnosis), using research versions of two common RNA-based prognostic assays: ROR-P and the 21-gene recurrence score (RS). Relative frequency differences and 95% CIs were estimated for associations with race and age, and hazards of 5-year local or distant recurrence were modeled with Cox regression. Proliferation and estrogen module scores from each assay, representing broad activity of genes in those pathways, were examined to guide interpretation of differences between tests.

RESULTS

Among both younger and older individuals, Black women had higher frequency of intermediate and high ROR-P scores than non-Black women. Race was not significantly associated with RS in either age group. High (hazard ratio [HR], 4.67 [95% CI, 1.73 to 12.70]) and intermediate (HR, 2.12 [95% CI, 0.98 to 4.62]) ROR-P scores were associated with greater risk of recurrence, but RS did not predict recurrence. RS emphasized estrogen over proliferation modules, whereas ROR-P emphasized proliferation. Higher proliferation scores were associated with younger age and Black race in both assays. Modifications to the RS algorithm that increased emphasis on proliferation improved prognostication in this diverse population.

CONCLUSION

ROR-P and the 21-gene RS differentially emphasize estrogen-related and proliferative biology. The emphasis of 21-gene RS on estrogen-related biology and lower endocrine therapy initiation among Black women may contribute to poorer prognostic ability in heterogeneously treated populations.

摘要

目的

基因组检测,如 Oncotype DX 21 基因和 Prosigna 复发风险(ROR-P)检测,常用于乳腺癌预后。新出现的数据表明检测之间存在差异,但尚未在不同人群中进行比较。

材料和方法

在 Carolina Breast Cancer Study 中,对 647 例先前未经治疗的 I-III 期雌激素受体阳性/人表皮生长因子受体 2 阴性肿瘤进行了 RNA 测序,该研究对黑人患者和年轻患者(诊断时年龄<50 岁)进行了过采样,并使用两种常见的基于 RNA 的预后检测的研究版本:ROR-P 和 21 基因复发评分(RS)。估计种族和年龄与这些检测之间的关联的相对频率差异和 95%置信区间,并使用 Cox 回归模型对 5 年局部或远处复发的风险进行建模。每个检测中代表这些途径中基因广泛活性的增殖和雌激素模块评分,用于指导检测之间差异的解释。

结果

在年轻和年长患者中,黑人女性的 ROR-P 评分中等到高度的频率均高于非黑人女性。在两个年龄组中,种族与 RS 均无显著相关性。高(危险比[HR],4.67[95%CI,1.73 至 12.70])和中(HR,2.12[95%CI,0.98 至 4.62])ROR-P 评分与更高的复发风险相关,但 RS 不能预测复发。RS 强调雌激素,而 ROR-P 强调增殖。在两个检测中,RS 强调雌激素,而 ROR-P 强调增殖。在两个检测中,高增殖评分与年轻年龄和黑人种族相关。在这个多样化的人群中,修改 RS 算法以增加对增殖的重视可提高预后。

结论

ROR-P 和 21 基因 RS 分别强调雌激素相关和增殖生物学。RS 对雌激素相关生物学的强调以及黑人女性中较低的内分泌治疗起始率可能导致在异质治疗人群中预后能力较差。

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