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三氟硝基咪唑作为实体瘤潜在缺氧报告分子的体内19F磁共振波谱和化学位移成像

In vivo 19F magnetic resonance spectroscopy and chemical shift imaging of tri-fluoro-nitroimidazole as a potential hypoxia reporter in solid tumors.

作者信息

Procissi Daniel, Claus Filip, Burgman Paul, Koziorowski Jacek, Chapman J Donald, Thakur Sunitha B, Matei Cornelia, Ling C Clifton, Koutcher Jason A

机构信息

Department of Medical Physics, Memorial Sloan-Kettering Cancer Center, New York, New York, USA.

出版信息

Clin Cancer Res. 2007 Jun 15;13(12):3738-47. doi: 10.1158/1078-0432.CCR-06-1563.

Abstract

PURPOSE

2-Nitro-alpha-[(2,2,2-trifluoroethoxy)methyl]-imidazole-1-ethanol (TF-MISO) was investigated as a potential noninvasive marker of tissue oxygen levels in tumors using (19)F magnetic resonance spectroscopy (MRS) and (19)F chemical shift imaging.

EXPERIMENTAL DESIGNS

In vitro data were obtained using high-performance liquid chromatography on tumor cells incubated under varying oxygen conditions to determine the oxygen-binding characteristics. In vivo data were obtained using a well-characterized hypoxic murine breast tumor (MCa), in addition to studies on a rat prostate tumor model (R3327-AT) implanted in nude mice. Detection of intratumor (19)F signal from TF-MISO was done using MRS for up to 10 h following a 75 mg/kg i.v. injection. Localized distribution of the compound in the implanted MCa tumor has been imaged using slice-selective two-dimensional chemical shift imaging 6 h after injection.

RESULTS

The in vitro results showed that TF-MISO preferentially accumulates in cells incubated under anoxic conditions. The in vivo (19)F MR spectral features (line width and chemical shift) were recorded as a function of time after injection, and the results indicate that the fluorine atoms are indeed sensitive to changes in the local environment while still providing a detectable MR signal. Ex vivo spectra were collected and established the visibility of the (19)F signal under conditions of maximum hypoxia. Late time point (>6 h) tumor tissue concentrations, as obtained from (19)F MRS, suggest that TF-MISO is reduced and retained in hypoxic tumor. The feasibility of obtaining TF-MISO tumor distribution maps in a reasonable time frame was established.

CONCLUSIONS

Based on the results presented herein, it is suggested that TF-MISO has the potential to be a valid magnetic resonance hypoxia imaging reporter for both preclinical hypoxia studies and hypoxia-directed clinical therapy.

摘要

目的

使用氟-19磁共振波谱(MRS)和氟-19化学位移成像,研究2-硝基-α-[(2,2,2-三氟乙氧基)甲基]-咪唑-1-乙醇(TF-MISO)作为肿瘤组织氧水平潜在无创标志物的情况。

实验设计

通过高效液相色谱法,在不同氧条件下孵育的肿瘤细胞上获取体外数据,以确定氧结合特性。除了对植入裸鼠的大鼠前列腺肿瘤模型(R3327-AT)进行研究外,还使用特征明确的缺氧小鼠乳腺肿瘤(MCa)获取体内数据。静脉注射75mg/kg后,使用MRS在长达10小时内检测TF-MISO的肿瘤内氟-19信号。注射后6小时,使用切片选择性二维化学位移成像对植入的MCa肿瘤中该化合物的局部分布进行成像。

结果

体外结果表明,TF-MISO优先积聚在缺氧条件下孵育的细胞中。记录了体内氟-19磁共振波谱特征(线宽和化学位移)随注射后时间的变化,结果表明氟原子确实对局部环境变化敏感,同时仍能提供可检测的磁共振信号。收集了离体波谱并确定了在最大缺氧条件下氟-19信号的可见性。从氟-19 MRS获得的晚期时间点(>6小时)肿瘤组织浓度表明,TF-MISO在缺氧肿瘤中被还原并保留。确定了在合理时间范围内获得TF-MISO肿瘤分布图的可行性。

结论

基于本文给出的结果,表明TF-MISO有潜力成为用于临床前缺氧研究和缺氧导向临床治疗的有效磁共振缺氧成像报告分子。

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