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三维共培养人胰腺癌细胞球的成球培养

Growing Desmoplastic Three-Dimensional Pancreatic Cancer Spheroids from Co-Culture.

机构信息

Department of Pharmaceutical Sciences, South Dakota State University.

Department of Pharmaceutical Sciences, South Dakota State University;

出版信息

J Vis Exp. 2024 Sep 27(211). doi: 10.3791/66625.

DOI:10.3791/66625
PMID:39400162
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is one of the deadliest cancers with a 5-year survival rate of <12%. The biggest barrier to therapy is the dense desmoplastic extracellular matrix (ECM) that surrounds the tumor and reduces vascularization, generally termed desmoplasia. A variety of drug combinations and formulations have been tested to treat the cancer, and although many of them show success pre-clinically, they fail clinically. It, therefore, becomes important to have a clinically relevant model available that can predict the response of the tumor to therapy. This model has been previously validated against resected clinical tumors. Here a simple protocol to grow desmoplastic three-dimensional (3D)-coculture spheroids is described that can naturally generating a robust ECM and do not require any external matrix sources or scaffold to support their growth. Briefly human pancreatic stellate cells (HPaSteC) and PANC-1 cells are used to prepare a suspension containing the cells in a 1:2 ratio, respectively. The cells are plated in a poly-HEMA coated, 96-well low attachment U-well plate. The plate is centrifuged to allow the cells to form an initial pellet. The plate is stored in the incubator at 37 °C with 5% CO2, and media is replaced every 3 days. Plates can be imaged at designated intervals to measure spheroid volume. Following 14 days of culture, mature desmoplastic spheroids are formed (i.e. average volume of 0.048 + 0.012 mm (451 µm x 462.84 µm)) and can be utilized for experimental therapy assessment. Mature ECM components include collagen-I, hyaluronic acid, fibronectin, and laminin.

摘要

胰腺导管腺癌 (PDAC) 是最致命的癌症之一,其 5 年生存率<12%。治疗的最大障碍是包围肿瘤并减少血管生成的致密细胞外基质 (ECM),通常称为纤维变性。已经测试了多种药物组合和制剂来治疗癌症,尽管其中许多在临床前显示出成功,但在临床上却失败了。因此,拥有一种可用于预测肿瘤对治疗反应的临床相关模型变得非常重要。该模型已经针对切除的临床肿瘤进行了验证。这里描述了一种简单的培养致密三维 (3D)-共培养球体的方案,该方案可以自然产生强大的 ECM,并且不需要任何外部基质源或支架来支持其生长。简要地说,人胰腺星状细胞 (HPaSteC) 和 PANC-1 细胞分别用于制备含有细胞的悬浮液,细胞比例为 1:2。将细胞接种在涂有多聚 HEPA 的 96 孔低附着 U 形孔板中。将平板离心以允许细胞形成初始沉淀。将平板在 37°C 下储存于 5%CO2 的孵育箱中,每 3 天更换一次培养基。可以在指定的时间间隔对平板进行成像以测量球体体积。培养 14 天后,形成成熟的纤维变性球体(即平均体积为 0.048+0.012mm(451µm x 462.84µm)),可用于实验治疗评估。成熟的 ECM 成分包括胶原-I、透明质酸、纤连蛋白和层粘连蛋白。

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引用本文的文献

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The type I collagen paradox in PDAC progression: microenvironmental protector turned tumor accomplice.胰腺癌进展中的I型胶原蛋白悖论:微环境保护者变成肿瘤帮凶。
J Transl Med. 2025 Jul 4;23(1):744. doi: 10.1186/s12967-025-06778-8.