A Novel Ex Vivo Tumor Spheroid-Tissue Model for Investigating Microvascular Remodeling and Lymphatic Blood Vessel Plasticity

IF 3 2区 医学 Q3 ENGINEERING, BIOMEDICAL Annals of Biomedical Engineering Pub Date : 2024-05-25 DOI:10.1007/s10439-024-03535-8
Arinola O. Lampejo, Suzanne E. Lightsey, Maria C. Gomes, Christian M. Nguyen, Dietmar W. Siemann, Blanka Sharma, Walter L. Murfee
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Abstract

Biomimetic tumor microenvironment models bridge the gap between in vitro and in vivo systems and serve as a useful way to address the modeling challenge of how to recreate the cell and system complexity associated with real tissues. Our laboratory has developed an ex vivo rat mesentery culture model, which allows for simultaneous investigation of blood and lymphatic microvascular network remodeling in an intact tissue environment. Given that angiogenesis and lymphangiogenesis are key contributors to the progression of cancer, the objective of this study was to combine tissue and tumor spheroid culture methods to establish a novel ex vivo tumor spheroid-tissue model by verifying its use for evaluating the effects of cancer cell behavior on the local microvascular environment. H1299 or A549 tumor spheroids were formed via hanging drop culture and seeded onto rat mesenteric tissues harvested from adult male Wistar rats. Tissues with transplanted spheroids were cultured in serum-free media for 3 to 5 days. PECAM, NG2, CD11b, and αSMA labeling identified endothelial cells, pericytes, immune cells, and smooth muscle cells, respectively. Time-lapse imaging confirmed cancer cell type specific migration. In addition to increasing PECAM positive capillary sprouting and LYVE-1 positive endothelial cell extensions indicative of lymphangiogenesis, tumor spheroid presence induced the formation of lymphatic/blood vessel connections and the formation of hybrid, mosaic vessels that were characterized by discontinuous LYVE-1 labeling. The results support the application of a novel tumor spheroid microenvironment model for investigating cancer cell–microvascular interactions.

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用于研究微血管重塑和淋巴管可塑性的新型体外肿瘤球形组织模型
仿生肿瘤微环境模型是体外和体内系统之间的桥梁,是解决如何再现与真实组织相关的细胞和系统复杂性这一建模难题的有效方法。我们的实验室开发了一种体外大鼠肠系膜培养模型,可以在完整的组织环境中同时研究血液和淋巴微血管网络的重塑。鉴于血管生成和淋巴管生成是癌症进展的关键因素,本研究的目的是结合组织和肿瘤球形培养方法,建立一种新型的体外肿瘤球形组织模型,验证其在评估癌细胞行为对局部微血管环境影响方面的用途。通过悬滴培养形成 H1299 或 A549 肿瘤球体,并将其播种到从成年雄性 Wistar 大鼠身上采集的大鼠肠系膜组织上。带有移植球的组织在无血清培养基中培养 3 至 5 天。PECAM、NG2、CD11b和αSMA标记分别确定了内皮细胞、周细胞、免疫细胞和平滑肌细胞。延时成像证实了癌细胞的特异性迁移。除了表明淋巴管生成的 PECAM 阳性毛细血管萌发和 LYVE-1 阳性内皮细胞延伸增加外,肿瘤球体的存在还诱导形成淋巴/血管连接,并形成以不连续 LYVE-1 标记为特征的混合、镶嵌血管。这些结果支持应用新型肿瘤球形体微环境模型来研究癌细胞与微血管之间的相互作用。
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来源期刊
Annals of Biomedical Engineering
Annals of Biomedical Engineering 工程技术-工程:生物医学
CiteScore
7.50
自引率
15.80%
发文量
212
审稿时长
3 months
期刊介绍: Annals of Biomedical Engineering is an official journal of the Biomedical Engineering Society, publishing original articles in the major fields of bioengineering and biomedical engineering. The Annals is an interdisciplinary and international journal with the aim to highlight integrated approaches to the solutions of biological and biomedical problems.
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