Seo Junki, Ha Giheon, Lee Geonho, Nasiri Rohollah, Lee Junmin
Division of Interdisciplinary Bioscience & Bioengineering, Pohang University of Science and Technology (POSTECH), Pohang 790-784, Republic of Korea.
Department of Materials Science and Engineering, Pohang University of Science and Technology (POSTECH), Pohang 790-784, Republic of Korea.
Acta Biomater. 2024 Dec;190:233-246. doi: 10.1016/j.actbio.2024.10.036. Epub 2024 Oct 24.
Tumor-associated macrophages (TAMs), as key components of tumor microenvironment (TME), exhibit phenotypic plasticity in response to environmental cues, causing polarization into either pro-inflammatory M1 phenotypes or immunosuppressive M2 phenotypes. Although TAM has been widely studied for its crucial involvement in the initiation, progression, metastasis, and immune regulation of cancer cells, there have been limited attempts to understand how the metastatic potentials of cancer cells influence TAM polarization within TME. Here, we developed a miniaturized TME model using a 3D hybrid system composed of murine melanoma cells and macrophages, aiming to investigate interactions between cancer cells exhibiting various metastatic potentials and macrophages within TME. The increase in spheroid size within this model was associated with a reduction in cancer cell viability. Examining macrophage surface marker expression and cytokine secretion indicated the development of diverse TMEs influenced by both spheroid size and the metastatic potential of cancer cells. Furthermore, a high-throughput microfluidic platform equipped with trapping systems and hybrid spheroids was employed to simulate the tumor-immune system of complex TMEs and for comparative analysis with traditional 3D culture models. This study provides insight into TAM polarization in melanoma with different heterogeneities by modeling cancer-immune systems, which can be potentially employed for immune-oncology research, drug screening, and personalized therapy. STATEMENT OF SIGNIFICANCE: This study presents the development of a 3D hybrid spheroid system designed to model tumor-immune interactions, providing a detailed analysis of how melanoma cell metastatic potential influences tumor-associated macrophage (TAM) polarization. By utilizing a microfluidic platform, we are able to replicate and investigate the complex tumor-immune system of the tumor microenvironments (TMEs) under continuous flow conditions. Our model holds significant potential for high-throughput drug screening and personalized medicine applications, offering a versatile tool for advancing cancer research and treatment strategies.
肿瘤相关巨噬细胞(TAM)作为肿瘤微环境(TME)的关键组成部分,会根据环境信号表现出表型可塑性,从而极化为促炎性M1表型或免疫抑制性M2表型。尽管TAM因其在癌细胞的起始、进展、转移和免疫调节中的关键作用而受到广泛研究,但对于癌细胞的转移潜能如何影响TME内的TAM极化,人们的了解还很有限。在此,我们利用由小鼠黑色素瘤细胞和巨噬细胞组成的3D混合系统开发了一个小型化的TME模型,旨在研究具有不同转移潜能的癌细胞与TME内巨噬细胞之间的相互作用。该模型中球体大小的增加与癌细胞活力的降低有关。对巨噬细胞表面标志物表达和细胞因子分泌的检测表明,受球体大小和癌细胞转移潜能影响,不同的TME得以形成。此外,还采用了配备捕获系统和混合球体的高通量微流控平台来模拟复杂TME的肿瘤免疫系统,并与传统3D培养模型进行比较分析。本研究通过构建癌症-免疫系统模型,深入了解了不同异质性黑色素瘤中的TAM极化情况,该模型有望用于免疫肿瘤学研究、药物筛选和个性化治疗。重要意义声明:本研究展示了一种用于模拟肿瘤-免疫相互作用 的3D混合球体系统的开发,详细分析了黑色素瘤细胞转移潜能如何影响肿瘤相关巨噬细胞(TAM)极化。通过利用微流控平台,我们能够在连续流动条件下复制和研究肿瘤微环境(TME)复杂的肿瘤-免疫系统。我们的模型在高通量药物筛选和个性化医疗应用方面具有巨大潜力,为推进癌症研究和治疗策略提供了一种多功能工具。
