Department of Cancer Genetics, Institute for Cancer Research, The Norwegian Radium Hospital, Oslo University Hospital, Norway.
Department of Tumor biology, Institute for Cancer Research, The Norwegian Radium Hospital, Oslo University Hospital, Norway.
Mol Oncol. 2019 Oct;13(10):2278-2296. doi: 10.1002/1878-0261.12561. Epub 2019 Aug 28.
One of the hallmarks of cancer is sustained angiogenesis. Favorable results have been reported in some breast cancer (BC) patients receiving antiangiogenic therapy with bevacizumab (Bev) in combination with chemotherapy, and further knowledge on how Bev can be optimally combined with conventional treatment to increase efficacy is strongly needed. In this randomized, neoadjuvant phase II clinical trial, 132 patients with HER2-negative, nonmetastatic BC were treated with Bev in combination with sequential chemotherapy. Biopsies were sampled before treatment, after 12 weeks with anthracycline and after taxane therapy at week 25. MicroRNA (miRNA) expression profiling was performed on biopsies from each time point. Altogether, 241 biopsies were analyzed with the aim of identifying miRNA-based biomarkers of response to therapy. Results from the miRNA analyses were reported for the ER-positive cohort, which were previously demonstrated to benefit from antiangiogenic therapy in this study. For both treatment arms of this cohort, significantly different expression was observed for 217 miRNAs between objective responding and nonresponding patients before treatment initiation. These miRNAs have been linked to regulation of epithelial-mesenchymal transition, metastasis, and tumor growth, among other processes. Bev in combination with chemotherapy resulted in similar miRNA changes to chemotherapy alone. However, the deregulation of miRNA expression occurred earlier in the Bev arm. In both arms, tumor suppressor miRNAs were found upregulated after treatment, while oncogenic miRNAs were downregulated in the Bev arm. Patients responding to Bev showed a strong correlation between deregulated miRNAs and decreased proliferation score during the course of treatment, with downregulation of miR-4465 as the strongest indicator of reduced proliferation. Integrative analyses at miRNA-, gene-, and protein expression further indicated a longitudinal decrease in proliferation. Altogether, the results indicate that proliferation might represent a predictive factor for increased Bev sensitivity, which may aid in the identification of patients who could potentially benefit from Bev.
癌症的一个特征是持续的血管生成。在一些接受贝伐单抗(Bev)联合化疗的乳腺癌(BC)患者中,已经报道了有利的结果,并且强烈需要进一步了解如何将 Bev 与常规治疗最佳结合以提高疗效。在这项随机、新辅助 II 期临床试验中,132 名 HER2 阴性、非转移性 BC 患者接受 Bev 联合序贯化疗治疗。在治疗前、第 12 周接受蒽环类药物治疗后和第 25 周接受紫杉烷治疗后进行活检取样。对每个时间点的活检进行 microRNA(miRNA)表达谱分析。总共分析了 241 个活检样本,目的是确定对治疗有反应的 miRNA 生物标志物。这些 miRNA 分析结果报告了 ER 阳性队列的结果,该队列在这项研究中先前被证明受益于抗血管生成治疗。对于该队列的两个治疗臂,在开始治疗前,217 个 miRNA 在客观反应和无反应患者之间的表达存在显著差异。这些 miRNA 与上皮-间充质转化、转移和肿瘤生长等过程的调节有关。Bev 联合化疗与单独化疗相比导致类似的 miRNA 变化。然而,Bev 臂中的 miRNA 表达失调发生得更早。在两个臂中,在治疗后发现肿瘤抑制 miRNA 上调,而在 Bev 臂中致癌 miRNA 下调。对 Bev 有反应的患者显示出在治疗过程中,miRNA 失调与增殖评分降低之间存在很强的相关性,miR-4465 的下调是增殖减少的最强指标。miRNA-、基因-和蛋白质表达的综合分析进一步表明增殖呈纵向下降。总的来说,这些结果表明增殖可能代表对 Bev 敏感性增加的预测因素,这可能有助于识别可能从 Bev 中受益的患者。
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