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活体动物肿瘤缺氧的光学成像及一种靶向缺氧药物疗效的评估。

Optical imaging of tumor hypoxia and evaluation of efficacy of a hypoxia-targeting drug in living animals.

作者信息

Harada Hiroshi, Kizaka-Kondoh Shinae, Hiraoka Masahiro

机构信息

Kyoto University Graduate School of Medicine, Japan.

出版信息

Mol Imaging. 2005 Jul-Sep;4(3):182-93. doi: 10.1162/15353500200505112.

Abstract

Solid tumors containing more hypoxic regions show a more malignant phenotype by increasing the expression of genes encoding angiogenic and metastatic factors. Hypoxia-inducible factor-1 (HIF-1) is a master transcriptional activator of such genes, and thus, imaging and targeting hypoxic tumor cells where HIF-1 is active are important in cancer therapy. In the present study, HIF-1 activity was monitored via an optical in vivo imaging system by using a luciferase reporter gene under the regulation of an artificial HIF-1-dependent promoter, 5HRE. To monitor tumor hypoxia, we isolated a stable reporter-transfectant, HeLa/5HRE-Luc, which expressed more than 100-fold luciferase in response to hypoxic stress, and observed bioluminescence from its xenografts. Immunohistochemical analysis of the xenografts with a hypoxia marker, pimonidazole, confirmed that the luciferase-expressing cells were hypoxic. Evaluation of the efficacy of a hypoxia-targeting prodrug, TOP3, using this optical imaging system revealed that hypoxic cells were significantly diminished by TOP3 treatment. Immunohistochemical analysis of the TOP3-treated xenografts confirmed that hypoxic cells underwent apoptosis and were removed after TOP3 treatment. These results demonstrate that this model system using the 5HRE-luciferase reporter construct provides qualitative information (hypoxic status) of solid tumors and enables one to conveniently evaluate the efficacy of cancer therapy on hypoxia in malignant solid tumors.

摘要

含有更多缺氧区域的实体瘤通过增加编码血管生成和转移因子的基因表达而表现出更恶性的表型。缺氧诱导因子-1(HIF-1)是此类基因的主要转录激活因子,因此,对HIF-1活跃的缺氧肿瘤细胞进行成像和靶向在癌症治疗中很重要。在本研究中,通过使用在人工HIF-1依赖性启动子5HRE调控下的荧光素酶报告基因,经由光学体内成像系统监测HIF-1活性。为了监测肿瘤缺氧情况,我们分离出一个稳定的报告基因转染细胞系HeLa/5HRE-Luc,其在缺氧应激下表达的荧光素酶比正常情况高出100倍以上,并观察了其异种移植瘤的生物发光情况。用缺氧标记物匹莫硝唑对异种移植瘤进行免疫组织化学分析,证实表达荧光素酶的细胞处于缺氧状态。使用该光学成像系统评估缺氧靶向前药TOP3的疗效,结果显示TOP3处理后缺氧细胞显著减少。对经TOP3处理的异种移植瘤进行免疫组织化学分析证实,缺氧细胞在TOP3处理后发生凋亡并被清除。这些结果表明,使用5HRE-荧光素酶报告构建体的该模型系统可提供实体瘤的定性信息(缺氧状态),并能够方便地评估癌症治疗对恶性实体瘤缺氧情况的疗效。

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