Preoperative β-Blockade with Propranolol Reduces Biomarkers of Metastasis in Breast Cancer: A Phase II Randomized Trial

医学 普萘洛尔 乳腺癌 转移 转移性乳腺癌 封锁 临床终点 索拉非尼 内科学 原发性肿瘤 肿瘤科 癌症 临床试验 受体 肝细胞癌
作者
Jonathan G. Hiller,Steve W. Cole,Elizabeth M. Crone,David J. Byrne,David M. Shackleford,Jia-Min B. Pang,Michael A. Henderson,Sophie Nightingale,Kwok M. Ho,Paul S. Myles,Stephen B. Fox,Bernhard Riedel,Erica K. Sloan
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:26 (8): 1803-1811 被引量:166
标识
DOI:10.1158/1078-0432.ccr-19-2641
摘要

Abstract Purpose: The majority of deaths from breast cancer occur following the development of metastatic disease, a process inhibited by β-blockers in preclinical studies. This phase II randomized controlled trial evaluated the effect of preoperative β-blockade with propranolol on biomarkers of metastatic potential and the immune cell profile within the primary tumor of patients with breast cancer. Patients and Methods: In this triple-blind placebo-controlled clinical trial, 60 patients were randomly assigned to receive an escalating dose of oral propranolol (n = 30; 80–160 mg daily) or placebo (n = 30) for 7 days prior to surgery. The primary endpoint investigated the effect of propranolol on prometastatic and proinflammatory gene expression within the primary tumor. Results: Propranolol downregulated primary tumor expression of mesenchymal genes (P = 0.002) without affecting epithelial gene expression (P = 0.21). Bioinformatic analyses implicated downregulation of Snail/Slug (P = 0.03), NF-κB/Rel (P < 0.01), and AP-1 (P < 0.01) transcription factors in structuring the observed transcriptome alterations, and identified changes in intratumoral neutrophil, natural killer cell, and dendritic cell recruitment (all P < 0.01). Patients with clinical evidence of drug response (lowered heart rate and blood pressure) demonstrated elevated tumor infiltration of CD68+ macrophages and CD8+ T cells. Conclusions: One week of β-blockade with propranolol reduced intratumoral mesenchymal polarization and promoted immune cell infiltration in early-stage surgically-resectable breast cancer. These results show that β-blockade reduces biomarkers associated with metastatic potential, and support the need for larger phase III clinical trials powered to detect the impact of β-blockade on cancer recurrence and survival. See related commentary by Blaes et al., p. 1781
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