Dana-Farber/Boston Children's Cancer and Blood Disorders Center, Boston, Massachusetts.
National Center for Advancing Translational Sciences, National Institutes of Health, Rockville, Maryland.
Clin Cancer Res. 2019 Jul 15;25(14):4552-4566. doi: 10.1158/1078-0432.CCR-17-0375. Epub 2019 Apr 12.
Ewing sarcoma is an aggressive solid tumor malignancy of childhood. Although current treatment regimens cure approximately 70% of patients with localized disease, they are ineffective for most patients with metastases or relapse. New treatment combinations are necessary for these patients.
Ewing sarcoma cells are dependent on focal adhesion kinase (FAK) for growth. To identify candidate treatment combinations for Ewing sarcoma, we performed a small-molecule library screen to identify compounds synergistic with FAK inhibitors in impairing Ewing cell growth. The activity of a top-scoring class of compounds was then validated across multiple Ewing cell lines and in multiple xenograft models of Ewing sarcoma.
Numerous Aurora kinase inhibitors scored as synergistic with FAK inhibition in this screen. We found that Aurora kinase B inhibitors were synergistic across a larger range of concentrations than Aurora kinase A inhibitors when combined with FAK inhibitors in multiple Ewing cell lines. The combination of AZD-1152, an Aurora kinase B-selective inhibitor, and PF-562271 or VS-4718, FAK-selective inhibitors, induced apoptosis in Ewing sarcoma cells at concentrations that had minimal effects on survival when cells were treated with either drug alone. We also found that the combination significantly impaired tumor progression in multiple xenograft models of Ewing sarcoma.
FAK and Aurora kinase B inhibitors synergistically impair Ewing sarcoma cell viability and significantly inhibit tumor progression. This study provides preclinical support for the consideration of a clinical trial testing the safety and efficacy of this combination for patients with Ewing sarcoma.
尤文肉瘤是一种儿童期侵袭性实体肿瘤恶性肿瘤。尽管目前的治疗方案可以治愈大约 70%的局限性疾病患者,但对于大多数转移性或复发性患者却无效。这些患者需要新的治疗组合。
尤文肉瘤细胞的生长依赖于粘着斑激酶(FAK)。为了确定尤文肉瘤的候选治疗组合,我们进行了小分子文库筛选,以鉴定与 FAK 抑制剂协同作用以损害尤文细胞生长的化合物。然后在多个尤文细胞系和多个尤文肉瘤异种移植模型中验证了得分最高的一类化合物的活性。
在该筛选中,许多 Aurora 激酶抑制剂被评为与 FAK 抑制协同作用。我们发现,与 Aurora 激酶 A 抑制剂相比,Aurora 激酶 B 抑制剂在与 FAK 抑制剂联合使用时,在多个尤文细胞系中以更大的浓度范围协同作用。Aurora 激酶 B 选择性抑制剂 AZD-1152 与 FAK 选择性抑制剂 PF-562271 或 VS-4718 的组合,在浓度诱导尤文肉瘤细胞凋亡,而当细胞单独用任一药物处理时,对存活的影响最小。我们还发现该组合显著抑制了多个尤文肉瘤异种移植模型中的肿瘤进展。
FAK 和 Aurora 激酶 B 抑制剂协同地损害尤文肉瘤细胞活力,并显著抑制肿瘤进展。这项研究为考虑临床试验测试该组合对尤文肉瘤患者的安全性和疗效提供了临床前支持。
