Department of Surgery, Medical University of Vienna, A-1090, Vienna, Austria.
Br J Cancer. 2010 Oct 12;103(8):1201-8. doi: 10.1038/sj.bjc.6605909. Epub 2010 Sep 28.
Despite the widespread use of neoadjuvant chemotherapy in breast cancer patients, prediction of individual response to treatment remains an unsolved clinical problem. Particularly, administration of an inefficient chemotherapeutic regimen should be avoided. Therefore, a better understanding of the molecular mechanisms underlying response to neoadjuvant chemotherapy is of particular clinical interest. Aim of the present study was to test whether neoadjuvant chemotherapy with epirubicin/docetaxel induces early changes in the plasma proteome of breast cancer patients and whether such changes correlate with response to therapy.
Plasma samples of 25 breast cancer patients obtained before and 24 h after initiation of epirubicin/docetaxel-based neoadjuvant chemotherapy were analysed using two-dimensional differential gel electrophoresis (2D-DIGE). Protein spots found to be differentially expressed were identified using mass spectrometry and then correlated with the pathological response after six cycles of therapy. Markers identified in a discovery set of patients (n=12) were confirmed in an independent validation set (n=13).
2D-DIGE revealed 33 protein spots to be differentially expressed in response to chemotherapy, including the complement factors C1, C3 and C4, inter-α-trypsin inhibitor, α-1-antichymotrypsin and α-2-Heremans-Schmid glycoprotein (AHSG). With respect to cytokines, only interleukin (IL)-6, IL-10 and soluble intracellular adgesion molecule 3 (sICAM3) were minimally modulated. Moreover, two protein spots within the complement component C3 significantly correlated with response to therapy.
We have identified acute phase proteins and the complement system as part of the early host response to epirubicin/docetaxel chemotherapy. As complement C3 cleavage correlates with the efficacy of docetaxel/epirubicin-based chemotherapy, it has the potential as an easily accessible predictive biomarker.
尽管新辅助化疗在乳腺癌患者中广泛应用,但预测个体对治疗的反应仍然是一个未解决的临床问题。特别是,应避免使用低效的化疗方案。因此,更好地了解新辅助化疗反应的分子机制具有特殊的临床意义。本研究的目的是检测表柔比星/多西紫杉醇新辅助化疗是否会引起乳腺癌患者血浆蛋白质组的早期变化,以及这些变化是否与治疗反应相关。
采用二维差异凝胶电泳(2D-DIGE)分析 25 例乳腺癌患者在开始表柔比星/多西紫杉醇新辅助化疗前和化疗 24 小时后的血浆样本。使用质谱法鉴定出差异表达的蛋白质斑点,然后将其与 6 个周期治疗后的病理反应相关联。在发现组患者(n=12)中鉴定出的标志物在独立验证组患者(n=13)中得到了验证。
2D-DIGE 显示 33 个蛋白质斑点对化疗有差异表达,包括补体因子 C1、C3 和 C4、α-1-抗胰蛋白酶、α-1-抗糜蛋白酶和α-2-赫姆斯曼-施密特糖蛋白(AHSG)。就细胞因子而言,只有白细胞介素(IL)-6、IL-10 和可溶性细胞内粘附分子 3(sICAM3)有轻微的调节。此外,补体成分 C3 内的两个蛋白质斑点与治疗反应显著相关。
我们已经确定了急性期蛋白和补体系统是表柔比星/多西紫杉醇化疗后早期宿主反应的一部分。由于补体 C3 裂解与多西紫杉醇/表柔比星化疗的疗效相关,因此它有可能成为一种易于获得的预测性生物标志物。
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