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首页> 外文期刊>The oncologist >Agreement in risk prediction between the 21-gene recurrence score assay (Oncotype DX?) and the PAM50 breast cancer intrinsic classifier ? in early-stage estrogen receptor-positive breast cancer
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Agreement in risk prediction between the 21-gene recurrence score assay (Oncotype DX?) and the PAM50 breast cancer intrinsic classifier ? in early-stage estrogen receptor-positive breast cancer

机译:21基因复发评分测定法(Oncotype DX?)与PAM50乳腺癌固有分类器之间的风险预测一致在早期雌激素受体阳性乳腺癌中

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Purpose. To compare risk assignment by PAM50 Breast Cancer Intrinsic Classifier ? and Oncotype DX_Recur-rence Score (RS) in the same population. Methods. RNA was extracted from 151 estrogen receptor (ER) + stage I-II breast cancers and gene expression profiled using PAM50 "intrinsic" subtyping test. Results. One hundred eight cases had complete molecular information; 103 (95%) were classified as luminal A (n = 76) or luminal B (n = 27). Ninety-two percent (n = 98) had a low (n = 59) or intermediate (n = 39) RS. Among luminal A cancers, 70% had low (n = 53) and the remainder (n = 23) had an intermediate RS. Among luminal B cancers, nine were high (33%) and 13 were intermediate (48%) by the RS. Almost all cancers with a high RS were classified as luminal B (90%, n = 9). One high RS cancer was identified as basal-like and had low ER/ESR1 and low human epidermal growth factor receptor 2 (HER2) expression by quantitative polymerase chain reaction in both assays. The majority of low RS cases were luminal A (83%, n = 53). Importantly, half of the intermediate RS cancers were re-categorized as low risk luminal A subtype by PAM50. Conclusion. There is good agreement between the two assays for high (i.e., luminal B or RS 31) and low (i.e., luminal B or RS 18) prognostic risk assignment but PAM50 assigns more patients to the low risk category. About half of the intermediate RS group was reclassified as luminal A by PAM50.
机译:目的。比较PAM50乳腺癌固有分类器的风险分配?和相同人群中的癌型DX_递归得分(RS)。方法。从151种雌激素受体(ER)+ I-II期乳腺癌中提取RNA,并使用PAM50“本征”亚型测试对基因表达进行分析。结果。一百零八例具有完整的分子信息。 103(95%)被分为管腔A(n = 76)或管腔B(n = 27)。 92%(n = 98)的RS低(n = 59)或中等(n = 39)。在管腔A型癌症中,有70%的癌症为低(n = 53),其余的癌症(n = 23)为中度RS。在管腔B型癌症中,RS导致9例高发(33%),中度13例(48%)。几乎所有具有高RS的癌症都归为B腔(90%,n = 9)。通过两种方法中的定量聚合酶链反应,一种高RS癌被鉴定为基底样,并且具有低ER / ESR1和低人表皮生长因子受体2(HER2)表达。大多数低RS病例是管腔A(83%,n = 53)。重要的是,PAM50将一半的中间RS癌症重新归类为低风险腔A型。结论。两种检测方法对高(即管腔B或RS> 31)和低(即管腔B或RS <18)的预后风险分配具有良好的一致性,但PAM50将更多的患者分配到低风险类别。 PAM50将大约一半的中间RS组重新分类为腔A。

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