van der Ent Wietske, Burrello Claudia, de Lange Mark J, van der Velden Pieter A, Jochemsen Aart G, Jager Martine J, Snaar-Jagalska B Ewa
Institute of Biology, Leiden University, Leiden University Medical Center, Leiden, The Netherlands; Department of Pathology, Leiden University Medical Center, Leiden, The Netherlands.
Institute of Biology, Leiden University, Leiden University Medical Center, Leiden, The Netherlands.
Ocul Oncol Pathol. 2015 Apr;1(3):170-81. doi: 10.1159/000370159. Epub 2015 Apr 9.
Although murine xenograft models for human uveal melanoma (UM) are available, they are of limited utility for screening large compound libraries for the discovery of new drugs. We need new preclinical models which can efficiently evaluate drugs that can treat UM metastases. The zebrafish embryonic model is ideal for drug screening purposes because it allows the investigation of potential antitumor properties of drugs within 1 week. The optical transparency of the zebrafish provides unique possibilities for live imaging of fluorescence-labelled cancer cells and their behavior. In addition, the adaptive immune response, which is responsible for the rejection of transplanted material, is not yet present in the early stages of fish development, and systemic immunosuppression is therefore not required to allow growth of tumor cells. We studied the behavior of UM cells following injection into zebrafish embryos and observed different phenotypes. We also analyzed cell migration, proliferation, formation of micrometastasis and interaction with the host microenvironment. Significant differences were noted between cell lines: cells derived from metastases showed more migration and proliferation than cells derived from the primary tumors. The addition of the c-Met inhibitor crizotinib to the water in which the larvae were kept reduced the migration and proliferation of UM cells expressing c-Met. This indicates the applicability of the zebrafish xenografts for testing novel inhibitory compounds and provides a fast and sensitive in vivo vertebrate model for preclinical drug screening to combat UM.
尽管有用于人类葡萄膜黑色素瘤(UM)的小鼠异种移植模型,但它们在筛选大型化合物文库以发现新药方面的效用有限。我们需要新的临床前模型,能够有效评估可治疗UM转移的药物。斑马鱼胚胎模型非常适合用于药物筛选,因为它能在1周内研究药物的潜在抗肿瘤特性。斑马鱼的光学透明性为荧光标记癌细胞及其行为的活体成像提供了独特的可能性。此外,负责排斥移植材料的适应性免疫反应在鱼类发育早期并不存在,因此无需进行全身免疫抑制就能使肿瘤细胞生长。我们研究了将UM细胞注射到斑马鱼胚胎后的行为,并观察到不同的表型。我们还分析了细胞迁移、增殖、微转移的形成以及与宿主微环境的相互作用。不同细胞系之间存在显著差异:源自转移灶的细胞比源自原发性肿瘤的细胞表现出更多的迁移和增殖。在饲养幼虫的水中添加c-Met抑制剂克唑替尼可减少表达c-Met的UM细胞的迁移和增殖。这表明斑马鱼异种移植在测试新型抑制性化合物方面的适用性,并为对抗UM的临床前药物筛选提供了一种快速且敏感的体内脊椎动物模型。