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六种癌症适应症来源的类肿瘤中患者特异性特征的长期维持。

Long-term maintenance of patient-specific characteristics in tumoroids from six cancer indications.

作者信息

Paul Colin D, Yankaskas Chris, Shahi Thakuri Pradip, Balhouse Brittany, Salen Shyanne, Bullock Amber, Beam Sylvia, Chatman Anthony, Djikeng Sybelle, Yang Xiaoyu Jenny, Wong Garrett, Dey Isha, Holmes Spencer, Dockey Abigail, Bailey-Steinitz Lindsay, Zheng Lina, Li Weizhong, Chandra Vivek, Nguyen Jakhan, Sharp Jason, Willems Erik, Kennedy Mark, Dallas Matthew R, Kuninger David

机构信息

Thermo Fisher Scientific, Frederick, MD, USA.

Thermo Fisher Scientific, Carlsbad, CA, USA.

出版信息

Sci Rep. 2025 Jan 31;15(1):3933. doi: 10.1038/s41598-025-86979-9.

Abstract

Tumoroids, sometimes referred to as cancer organoids, are patient-derived cancer cells grown as 3D, self-organized multicellular structures that maintain key characteristics (e.g., genotype, gene expression levels) of the tumor from which they originated. These models have emerged as valuable tools for studying tumor biology, cytotoxicity, and response of patient-derived cells to cancer therapies. However, the establishment and maintenance of tumoroids has historically been challenging, labor intensive, and highly variable from lab to lab, hindering their widespread use. Here, we characterize the establishment and/or expansion of colorectal, lung, head and neck, breast, pancreas, and endometrial tumoroids using the standardized, serum-free Gibco OncoPro Tumoroid Culture Medium. Newly derived tumoroid lines (n = 20) were analyzed by targeted genomic profiling and RNA sequencing and were representative of tumor tissue samples. Tumoroid lines were stable for over 250 days in culture and freeze-thaw competent. Previously established tumoroid lines were also transitioned to OncoPro medium and exhibited, on average, similar growth rates and conserved donor-specific characteristics when compared to original media systems. Additionally, OncoPro medium was compatible with both embedded culture in extracellular matrix and growth in a suspension format for facile culture and scale up. An example application of these models for assessing the cytotoxicity of a natural killer cell line and primary natural killer cells over time and at various doses demonstrated the compatibility of these models with assays used in compound and cell therapy development. We anticipate that the standardization and versatility of this approach will have important benefits for basic cancer research, drug discovery, and personalized medicine and help make tumoroid models more accessible to the cancer research community.

摘要

肿瘤类器官,有时也被称为癌症类器官,是源自患者的癌细胞,生长为三维、自组织的多细胞结构,保留了其起源肿瘤的关键特征(如基因型、基因表达水平)。这些模型已成为研究肿瘤生物学、细胞毒性以及患者来源细胞对癌症治疗反应的有价值工具。然而,肿瘤类器官的建立和维持历来具有挑战性, labor intensive,且实验室之间差异很大,阻碍了它们的广泛应用。在这里,我们使用标准化的无血清Gibco OncoPro肿瘤类器官培养基来描述结直肠癌、肺癌、头颈癌、乳腺癌、胰腺癌和子宫内膜癌肿瘤类器官的建立和/或扩增情况。通过靶向基因组分析和RNA测序对新建立的肿瘤类器官系(n = 20)进行了分析,这些系代表了肿瘤组织样本。肿瘤类器官系在培养中稳定超过250天,并且能够冻融。先前建立的肿瘤类器官系也转换到OncoPro培养基中,与原始培养基系统相比,平均表现出相似的生长速率并保留了供体特异性特征。此外,OncoPro培养基与细胞外基质包埋培养和悬浮培养形式均兼容,便于培养和扩大规模。这些模型用于评估自然杀伤细胞系和原代自然杀伤细胞在不同时间和不同剂量下的细胞毒性的一个示例应用,证明了这些模型与化合物和细胞疗法开发中使用的检测方法的兼容性。我们预计,这种方法的标准化和通用性将对基础癌症研究、药物发现和个性化医疗产生重要益处,并有助于使肿瘤类器官模型更易于癌症研究界使用。 (注:原文中“labor intensive”未翻译完整,其常见释义为“劳动密集型的” )

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1e70/11785764/4f504020e0c2/41598_2025_86979_Fig1_HTML.jpg

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