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二乙酰双(N(4)-甲基硫代半卡巴腙)铜的肿瘤摄取:组织氧合变化的影响

Tumor uptake of copper-diacetyl-bis(N(4)-methylthiosemicarbazone): effect of changes in tissue oxygenation.

作者信息

Lewis J S, Sharp T L, Laforest R, Fujibayashi Y, Welch M J

机构信息

Mallinckrodt Institute of Radiology, Washington University School of Medicine, St. Louis, Missouri, USA.

出版信息

J Nucl Med. 2001 Apr;42(4):655-61.

Abstract

UNLABELLED

We showed previously that, in vitro, copper-diacetyl-bis(N(4)-methylthiosemicarbazone) (Cu-ATSM) uptake is dependent on the oxygen concentration (pO2). We also showed that, in vivo, Cu-ATSM uptake is heterogeneous in animal tumors known to contain hypoxic fractions. This study was undertaken to confirm the pO2 dependence of this selective uptake in vivo by correlating Cu-ATSM uptake with measured tumor pO2.

METHODS

Experiments were performed with the 9L gliosarcoma rat model using a needle oxygen electrode to measure tissue pO2. Using PET and electronic autoradiography, Cu-ATSM uptake was measured in tumor tissue under various pO2 levels. The oxygen concentration within implanted tumors was manipulated by chemical means or by altering the inhaled oxygen content.

RESULTS

A good correlation between low pO2 and high Cu-ATSM accumulation was observed. Hydralazine administration in animals caused a decrease in the average tumor pO2 from 28.61 +/- 8.74 mm Hg to 20.81 +/- 7.54 mm Hg in untreated control animals breathing atmospheric oxygen. It also caused the tumor uptake of Cu-ATSM to increase by 35%. Conversely, in animals breathing 100% oxygen, the average tumor pO2 increased to 45.88 +/-15.9 mm Hg, and the tumor uptake of Cu-ATSM decreased to 48% of that of the control animals. PET of animals treated in a similar fashion yielded time-activity curves showing significantly higher retention of the tracer in hypoxic tissues than in oxygenated tissues.

CONCLUSION

These data confirm that Cu-ATSM uptake in tissues in vivo is dependent on the tissue pO2, and that significantly greater uptake and retention occur in hypoxic tumor tissue. Therefore, the possible use of Cu-ATSM PET as a prognostic indicator in the management of cancer is further validated.

摘要

未标记

我们之前表明,在体外,双乙酰双(N(4)-甲基硫代氨基脲)铜(Cu-ATSM)的摄取取决于氧浓度(pO₂)。我们还表明,在体内,已知含有缺氧部分的动物肿瘤中Cu-ATSM的摄取是异质性的。本研究旨在通过将Cu-ATSM摄取与测量的肿瘤pO₂相关联,来证实这种选择性摄取在体内对pO₂的依赖性。

方法

使用针式氧电极测量组织pO₂,在9L胶质肉瘤大鼠模型上进行实验。利用正电子发射断层扫描(PET)和电子放射自显影术,在不同pO₂水平下测量肿瘤组织中Cu-ATSM的摄取。通过化学方法或改变吸入氧含量来控制植入肿瘤内的氧浓度。

结果

观察到低pO₂与高Cu-ATSM积累之间存在良好的相关性。在呼吸大气氧的未治疗对照动物中,给动物施用肼导致平均肿瘤pO₂从28.61±8.74毫米汞柱降至20.81±7.54毫米汞柱。这也导致肿瘤对Cu-ATSM的摄取增加了35%。相反,在呼吸100%氧的动物中,平均肿瘤pO₂升至45.88±15.9毫米汞柱,肿瘤对Cu-ATSM的摄取降至对照动物的48%。以类似方式处理的动物的PET产生的时间-活性曲线显示,示踪剂在缺氧组织中的滞留明显高于在含氧组织中的滞留。

结论

这些数据证实,体内组织中Cu-ATSM的摄取取决于组织pO₂,并且在缺氧肿瘤组织中的摄取和滞留明显更大。因此,Cu-ATSM PET作为癌症管理中预后指标的可能用途得到了进一步验证。

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