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通过19F磁共振波谱在体内证明氟化硝基咪唑探针的肿瘤选择性滞留。

Demonstration of tumor-selective retention of fluorinated nitroimidazole probes by 19F magnetic resonance spectroscopy in vivo.

作者信息

Maxwell R J, Workman P, Griffiths J R

机构信息

Department of Biochemistry, St George's Hospital Medical School, London, UK.

出版信息

Int J Radiat Oncol Biol Phys. 1989 Apr;16(4):925-9. doi: 10.1016/0360-3016(89)90888-2.

DOI:10.1016/0360-3016(89)90888-2
PMID:2703398
Abstract

We have evaluated two fluorinated misonidazole analogues, Ro 07-0741 and CCI-103F, as potential probes for the non-invasive identification of hypoxic tumor cells by 19F magnetic resonance spectroscopy (MRS) in vivo. The equipment used was a 1.9 T Oxford Research Systems TMR-32 spectrometer, fitted with a 15 mm diameter surface coil. Signal was readily detectable, with similar intensity from EMT6 tumor, liver, and brain at early times (1-2 hr) after i.v. injection in BALB/c mice, indicative of an initial uniform biodistribution of parent probes. At later times (5-10 hr) there was a progressive reduction in signal intensity from brain and liver, but tumor levels remained constant or declined more slowly. This is illustrated by tumor/brain ratios at 6-7 hr of 2.9 (Ro 07-0741) and 4.2 (CCI-103F). In 4/5 mice analyzed at 20-24 hr after Ro 07-0741, and 1/2 following CCI-103F, tumor signal remained detectable. This occurred in the absence of parent probe as measured by HPLC, suggesting the involvement of a product of nitroreductive bioactivation. Studies with KHT and RIF-1 tumors in C3H/He mice showed a similar trend but retention in RIF-1 was less dramatic, and this was consistent with the known hypoxic fractions and comparative in vivo nitroreductase activities. These promising results support the continuing development of 19F nitroimidazole probes for non-invasive identification of hypoxic cells in vivo.

摘要

我们评估了两种氟化米索硝唑类似物Ro 07-0741和CCI-103F,作为通过19F磁共振波谱(MRS)在体内非侵入性鉴定缺氧肿瘤细胞的潜在探针。所用设备为1.9 T牛津研究系统TMR-32光谱仪,配备直径15 mm的表面线圈。静脉注射后早期(1 - 2小时),BALB/c小鼠体内EMT6肿瘤、肝脏和大脑中的信号易于检测,强度相似,表明母体探针最初分布均匀。在后期(5 - 10小时),大脑和肝脏中的信号强度逐渐降低,但肿瘤中的信号水平保持不变或下降更慢。这通过6 - 7小时时的肿瘤/大脑比值得到说明,Ro 07-0741为2.9,CCI-103F为4.2。在Ro 07-0741注射后20 - 24小时分析的5只小鼠中有4只,CCI-103F注射后分析的2只小鼠中有1只,肿瘤信号仍可检测到。通过高效液相色谱法测量,这是在没有母体探针的情况下发生的,表明涉及硝基还原生物活化产物。对C3H/He小鼠的KHT和RIF-1肿瘤的研究显示了类似趋势,但RIF-1中的保留情况不那么明显,这与已知的缺氧分数和体内比较硝基还原酶活性一致。这些有前景的结果支持继续开发19F硝基咪唑探针用于体内缺氧细胞的非侵入性鉴定。

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