小鼠肿瘤模型对生物发光成像因子的免疫应答。

IF 2.5 4区医学 Q2 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING

Molecular Imaging and Biology Pub Date : 2025-06-01 Epub Date: 2025-04-15 DOI:10.1007/s11307-025-02010-7

Angisha Basnet, Dylan D Thomas, Kaitlyn M Landreth, F Heath Damron, Tracy W Liu

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引用次数: 0

摘要

目的：影像报告器已广泛应用于肿瘤研究，实时监测肿瘤负荷和转移扩散。这些工具为肿瘤动态的非侵入性成像提供了有价值的方法。随着对肿瘤免疫学在癌症进展中起关键作用的既定认识，确保选择用于研究肿瘤-免疫相互作用的成像报告不会无意中引起免疫反应是至关重要的。本研究旨在研究用于肿瘤细胞体内跟踪的生物发光报告在免疫功能小鼠模型中的免疫应答。方法：研究了稳定表达的两种生物发光报告基因（红移萤火虫荧光素酶和点击甲虫绿色荧光素酶）在四种不同癌细胞系中的体外和体内生长效果。使用流式细胞术、细胞因子阵列和elisa评估亲代和报告表达癌细胞免疫细胞组成、激活和分泌细胞因子水平的差异。结果：数据显示亲本和报告癌细胞系的体外细胞增殖无显著差异。在体内，稳定表达红移萤火虫荧光素酶的肿瘤细胞未观察到皮下肿瘤的生长。用点击甲虫绿色荧光素酶标记的细胞与亲本细胞相比，在体内皮下肿瘤生长方面没有显着差异。与亲本和点击甲虫绿色荧光素酶相比，表达红移萤火虫荧光素酶的肿瘤细胞诱导激活和细胞毒性T细胞增加，表明免疫原性增强。此外，亲代和点击甲虫绿色荧光素酶标记的肿瘤细胞之间的肿瘤免疫组成和细胞因子产生相似。结论：这些发现表明，与红移萤火虫荧光素酶相比，点击甲虫绿色荧光素酶在癌细胞中的稳定表达具有最小的免疫原性，并且不会改变免疫功能正常小鼠的肿瘤发展。我们报告了生物发光报告细胞的详细表征研究，为它们在研究同基因小鼠肿瘤模型中肿瘤免疫相互作用提供了必要的考虑。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Immune Response to Bioluminescence Imaging Reporters in Murine Tumor Models.

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Immune Response to Bioluminescence Imaging Reporters in Murine Tumor Models.

Purpose: Imaging reporters have been widely employed in cancer research to monitor real-time tumor burden and metastatic spread. These tools offer a valuable approach for non-invasive imaging of tumor dynamics over time. With the established understanding that tumor immunology plays a critical role in cancer progression, it is essential to ensure that the chosen imaging reporters used to study tumor-immune interactions do not inadvertently elicit an immune response. This study aimed to investigate the immune response to bioluminescence reporters used for in vivo tracking of tumor cells in immunocompetent murine models.

Procedures: The in vitro and in vivo growth effects of two stably expressed bioluminescence reporter genes, a red-shifted firefly luciferase and a click beetle green luciferase, were evaluated in four different cancer cell lines. Differences in parental and reporter-expressing cancer cell immune cell composition, activation, and secreted cytokine levels were evaluated using flow cytometry, cytokine arrays and ELISAs.

Results: The data revealed no significant differences in in vitro cell proliferation between parental and reporter cancer cell lines. In vivo subcutaneous tumor growth was not observed in tumor cells stably expressing the red-shifted firefly luciferase. Cells labeled with click beetle green luciferase demonstrated no significant differences in in vivo subcutaneous tumor growth compared to parental cells. Tumor cells expressing red-shifted firefly luciferase induced an increase in activated and cytotoxic T cells compared to parental and click beetle green luciferase, suggesting enhanced immunogenicity. Furthermore, the tumor-immune composition and cytokine production were similar between parental and click beetle green luciferase-labeled tumor cells.

Conclusions: These findings demonstrate that the stable expression of click beetle green luciferase in cancer cells, in contrast to red-shifted firefly luciferase, has minimal immunogenicity and does not alter tumor development in immunocompetent mice. We report detailed characterization studies of bioluminescence reporter cells, providing essential considerations for their use in investigating tumor-immune interactions in syngeneic murine tumor models.

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来源期刊

Molecular Imaging and Biology 医学-核医学

CiteScore

6.90

自引率

3.20%

发文量

审稿时长

3 months

期刊介绍： Molecular Imaging and Biology (MIB) invites original contributions (research articles, review articles, commentaries, etc.) on the utilization of molecular imaging (i.e., nuclear imaging, optical imaging, autoradiography and pathology, MRI, MPI, ultrasound imaging, radiomics/genomics etc.) to investigate questions related to biology and health. The objective of MIB is to provide a forum to the discovery of molecular mechanisms of disease through the use of imaging techniques. We aim to investigate the biological nature of disease in patients and establish new molecular imaging diagnostic and therapy procedures. Some areas that are covered are: Preclinical and clinical imaging of macromolecular targets (e.g., genes, receptors, enzymes) involved in significant biological processes. The design, characterization, and study of new molecular imaging probes and contrast agents for the functional interrogation of macromolecular targets. Development and evaluation of imaging systems including instrumentation, image reconstruction algorithms, image analysis, and display. Development of molecular assay approaches leading to quantification of the biological information obtained in molecular imaging. Study of in vivo animal models of disease for the development of new molecular diagnostics and therapeutics. Extension of in vitro and in vivo discoveries using disease models, into well designed clinical research investigations. Clinical molecular imaging involving clinical investigations, clinical trials and medical management or cost-effectiveness studies.