Department of Medical Oncology & Therapeutics Research, City of Hope Cancer Center, Duarte, CA, 91010-3000, USA.
Breast Cancer Res Treat. 2011 Jul;128(1):155-63. doi: 10.1007/s10549-011-1508-0. Epub 2011 Apr 16.
Patients with locally advanced/inflammatory breast cancer (LABC/IBC) face a high likelyhood of recurrence and prognosis for relapsed, or de novo stage IV metastatic breast cancer (MBC) remains poor. Estrogen (ER) and HER2 receptor expression on primary or MBC allow targeted therapies, but an estimated 10-18% of tumors do not exhibit these biomarkers and survival in these cases is even poorer. Variations in discordance rates for the expression of ER and HER2 receptors have been observed between primary and metastatic tumors and such discordances may lead to suboptimal treatment. Circulating tumor cells (CTCs) are considered the seeds of residual disease and distant metastases and their characterization could help guide treatment selection. To explore this possibility, we used multiple biomarker assessment of CTCs in comparison to primary and metastatic tumor sites. Thirty-six patients with LABC/IBC, or stage IV MBC were evaluated. Blood samples were procured prior to initiating or changing therapy. CTCs were identified based on presence of cytokeratin and nucleus staining, and the absence of CD45. A multimarker assay was developed to simultaneously quantify expression of HER2, ER, and ERCC1, a DNA excision repair protein. Novel fiber-optic array scanning technology (FAST) was used for sensitive location of CTCs. CTCs were detected in 82% of MBC and 62% LABC/IBC cases. Multiplex marker expression was successfully carried out in samples from18 patients with MBC and in 8 patients with LABC/IBC that contained CTCs. In MBC, we detected actionable discordance rates of 40 and 23%, respectively for ER and HER2 where a biomarker was negative in the primary or metastatic tumor and positive in the CTCs. In LABC/IBC, actionable discordances were 60 and 20% for ER and HER2, respectively. Pilot trials evaluating the effectiveness of treatment selections based on actionable discordances between biomarker expression patterns on CTCs and primary or metastatic tumor sites may allow for a prospective assessment of CTC-based individualized targeted therapies.
局部晚期/炎症性乳腺癌(LABC/IBC)患者复发的可能性较高,且复发或初诊为 IV 期转移性乳腺癌(MBC)患者的预后仍然较差。原发或MBC 肿瘤的雌激素(ER)和 HER2 受体表达允许进行靶向治疗,但估计有 10-18%的肿瘤不表达这些生物标志物,这些情况下的生存率更差。原发和转移性肿瘤之间 ER 和 HER2 受体表达的不一致率存在差异,这种不一致可能导致治疗效果不佳。循环肿瘤细胞(CTC)被认为是残留疾病和远处转移的种子,其特征可帮助指导治疗选择。为了探索这种可能性,我们使用 CTC 多个生物标志物的评估,与原发和转移肿瘤部位进行了比较。评估了 36 例 LABC/IBC 或 IV 期 MBC 患者。在开始或改变治疗前采集血样。CTC 是基于存在细胞角蛋白和细胞核染色,且不存在 CD45 而鉴定的。开发了一种多标记物测定法,以同时定量 HER2、ER 和 ERCC1(一种 DNA 切除修复蛋白)的表达。新型光纤阵列扫描技术(FAST)用于敏感定位 CTCs。在 82%的 MBC 和 62%的 LABC/IBC 病例中检测到 CTCs。在 18 例 MBC 患者和 8 例含有 CTCs 的 LABC/IBC 患者的样本中成功进行了多重标记物表达。在 MBC 中,我们分别检测到 ER 和 HER2 的可操作不一致率为 40%和 23%,即生物标志物在原发或转移肿瘤中为阴性,而在 CTCs 中为阳性。在 LABC/IBC 中,ER 和 HER2 的可操作不一致率分别为 60%和 20%。评估基于 CTC 与原发或转移肿瘤部位之间的生物标志物表达模式的治疗选择有效性的初步试验,可能允许前瞻性评估基于 CTC 的个体化靶向治疗。
