Breast Cancer Unit, Department of Medical Oncology, Catalan Institute of Oncology (ICO), L'Hospitalet de Llobregat, Barcelona, Spain.
Department of Medical Oncology, Arnau de Vilanova University Hospital, Lleida, Spain.
Sci Rep. 2024 Oct 9;14(1):23626. doi: 10.1038/s41598-024-72152-1.
Neoadjuvant endocrine therapy (NET) for hormone receptor-positive (HR+) breast cancer might be as effective as chemotherapy, with a better toxicity profile. Blocking a crucial process such as angiogenesis with sunitinib may have a synergistic effect with NET. We aimed to assess the efficacy and safety of neoadjuvant sunitinib plus exemestane in early-stage HR+/HER2-negative breast cancer. In this phase I/II study, postmenopausal women with HR+/HER2- stage II-III breast cancer received neoadjuvant exemestane at conventional dose of 25mg plus sunitinib in a 3 + 3 design at 25mg (3/1weeks scheme) or 37.5mg continuous dose, for 6 months. Coprimary endpoints were the recommended dose of sunitinib combined with exemestane and objective response. Secondary endpoints included safety and biomarkers of early response. For 15 months, 18 patients were enrolled, 15 at sunitinib 25mg and 3 at 37.5mg. Median age was 73, 77% of patients had T2 tumors and 67% node-positive disease. The most common grade 2 toxicity was asthenia (44%), as was hypertension (22%) for grade 3. No grade 4-5 were reported. Twelve patients (66%) achieved an objective response. VEGFR-2 levels significantly decreased after one month of treatment. Differential gene expression analysis showed downregulation of ESR1, PGR and NAT1 in post-treatment samples and upregulation of EGFR, MYC, SFRP1, and FOXC1. PAM50 analysis on 83% of patients showed a prevalence of luminal A subtype, both in pre-treatment (63.6%) and post-treatment tumors (54.5%). Sunitinib plus exemestane was associated with substantial yet reversible toxicities, providing safety, efficacy and biological impact insights of combining an antiangiogenic drug with hormone therapy in early-stage breast cancer.Trial registration: Registered with ClinicalTrials.gov, NCT00931450. 02/07/2009.
新辅助内分泌治疗(NET)对于激素受体阳性(HR+)乳腺癌可能与化疗一样有效,且毒性更小。用舒尼替尼阻断血管生成等关键过程可能与 NET 具有协同作用。我们旨在评估新辅助舒尼替尼联合依西美坦治疗早期 HR+/HER2-阴性乳腺癌的疗效和安全性。在这项 I/II 期研究中,绝经后 HR+/HER2-Ⅱ-Ⅲ期乳腺癌患者接受常规剂量 25mg 的依西美坦联合舒尼替尼新辅助治疗,舒尼替尼采用 3+3 设计,剂量为 25mg(3/1 周方案)或 37.5mg 连续剂量,治疗 6 个月。主要终点为舒尼替尼联合依西美坦的推荐剂量和客观缓解。次要终点包括安全性和早期反应的生物标志物。在 15 个月期间,共入组了 18 例患者,其中舒尼替尼 25mg 组 15 例,37.5mg 组 3 例。中位年龄为 73 岁,77%的患者为 T2 肿瘤,67%的患者有淋巴结转移。最常见的 2 级毒性为乏力(44%),高血压为 3 级(22%)。无 4-5 级毒性。12 例患者(66%)达到客观缓解。治疗 1 个月后,VEGFR-2 水平显著下降。差异基因表达分析显示,治疗后样本中 ESR1、PGR 和 NAT1 下调,EGFR、MYC、SFRP1 和 FOXC1 上调。对 83%的患者进行 PAM50 分析显示,治疗前(63.6%)和治疗后肿瘤(54.5%)中均以 luminal A 亚型为主。舒尼替尼联合依西美坦治疗相关毒性较大,但可恢复,为联合抗血管生成药物与激素治疗早期乳腺癌的安全性、有效性和生物学影响提供了新的见解。试验注册:ClinicalTrials.gov 注册,NCT00931450。2009 年 7 月 2 日。
