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诱导性致癌肿瘤抗原的体内成像可观察肿瘤进展并预测 CTL 耐受。

In vivo imaging of an inducible oncogenic tumor antigen visualizes tumor progression and predicts CTL tolerance.

机构信息

Institute of Immunology, Charité Campus Benjamin Franklin, Berlin, Germany.

出版信息

J Immunol. 2010 Mar 15;184(6):2930-8. doi: 10.4049/jimmunol.0900893. Epub 2010 Feb 8.

Abstract

Visualizing oncogene/tumor Ag expression by noninvasive imaging is of great interest for understanding processes of tumor development and therapy. We established transgenic (Tg) mice conditionally expressing a fusion protein of the SV40 large T Ag and luciferase (TagLuc) that allows monitoring of oncogene/tumor Ag expression by bioluminescent imaging upon Cre recombinase-mediated activation. Independent of Cre-mediated recombination, the TagLuc gene was expressed at low levels in different tissues, probably due to the leakiness of the stop cassette. The level of spontaneous TagLuc expression, detected by bioluminescent imaging, varied between the different Tg lines, depended on the nature of the Tg expression cassette, and correlated with Tag-specific CTL tolerance. Following liver-specific Cre-loxP site-mediated excision of the stop cassette that separated the promoter from the TagLuc fusion gene, hepatocellular carcinoma development was visualized. The ubiquitous low level TagLuc expression caused the failure of transferred effector T cells to reject Tag-expressing tumors rather than causing graft-versus-host disease. This model may be useful to study different levels of tolerance, monitor tumor development at an early stage, and rapidly visualize the efficacy of therapeutic intervention versus potential side effects of low-level Ag expression in normal tissues.

摘要

通过非侵入性成像来可视化癌基因/肿瘤 Ag 的表达对于了解肿瘤发展和治疗过程具有重要意义。我们建立了条件性表达 SV40 大 T Ag 和荧光素酶融合蛋白的转基因 (Tg) 小鼠(TagLuc),该蛋白允许通过 Cre 重组酶介导的激活进行生物发光成像来监测癌基因/肿瘤 Ag 的表达。独立于 Cre 介导的重组,TagLuc 基因在不同组织中以低水平表达,这可能是由于终止盒的渗漏。通过生物发光成像检测到的自发 TagLuc 表达水平在不同的 Tg 系之间存在差异,这取决于 Tg 表达盒的性质,并与 Tag 特异性 CTL 耐受相关。在肝特异性 Cre-loxP 位点介导切除分离启动子和 TagLuc 融合基因的终止盒后,可可视化肝细胞癌的发展。普遍存在的低水平 TagLuc 表达导致转移效应 T 细胞无法排斥表达 Tag 的肿瘤,而不是引起移植物抗宿主病。该模型可能有助于研究不同水平的耐受,早期监测肿瘤发展,并快速可视化治疗干预的效果与正常组织中低水平 Ag 表达的潜在副作用。

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