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首页> 外文期刊>Journal of cellular and molecular medicine. >Impact of myo‐inositol trispyrophosphate (ITPP) on tumour oxygenation and response to irradiation in rodent tumour models
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Impact of myo‐inositol trispyrophosphate (ITPP) on tumour oxygenation and response to irradiation in rodent tumour models

机译:鼠肌瘤模型中肌醇三焦磷酸酯(ITPP)对肿瘤氧合和辐射响应的影响

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摘要

Tumour hypoxia is a well‐established factor of resistance in radiation therapy (RT). Myo ‐inositol trispyrophosphate (ITPP) is an allosteric effector that reduces the oxygen‐binding affinity of haemoglobin and facilitates the release of oxygen by red blood cells. We investigated herein the oxygenation effect of ITPP in six tumour models and its radiosensitizing effect in two of these models. The evolution of tumour pOsub2/sub upon ITPP administration was monitored on six models using 1.2?GHz Electron Paramagnetic Resonance (EPR) oximetry. The effect of ITPP on tumour perfusion was assessed by Hoechst staining and the oxygen consumption rate (OCR) in vitro was measured using 9.5?GHz EPR. The therapeutic effect of ITPP with and without RT was evaluated on rhabdomyosarcoma and 9L‐glioma rat models. ITPP enhanced tumour oxygenation in six models. The administration of 2?g/kg ITPP once daily for 2?days led to a tumour reoxygenation for at least 4?days. ITPP reduced the OCR in six cell lines but had no effect on tumour perfusion when tested on 9L‐gliomas. ITPP plus RT did not improve the outcome in rhabdomyosarcomas. In 9L‐gliomas, some of tumours receiving the combined treatment were cured while other tumours did not benefit from the treatment. ITPP increased oxygenation in six tumour models. A decrease in OCR could contribute to the decrease in tumour hypoxia. The association of RT with ITPP was beneficial for a few 9L‐gliomas but was absent in the rhabdomyosarcomas.
机译:肿瘤缺氧是放疗(RT)中公认的耐药因素。肌醇三焦磷酸酯(ITPP)是一种变构效应物,可降低血红蛋白的氧结合亲和力并促进红细胞释放氧。我们在这里研究了ITPP在六个肿瘤模型中的氧化作用及其在其中两个模型中的放射增敏作用。使用1.2?GHz电子顺磁共振(EPR)血氧测定法在六个模型上监测ITPP给药后肿瘤pO 2 的演变。通过Hoechst染色评估ITPP对肿瘤灌注的影响,并使用9.5?GHz EPR测量体外耗氧率(OCR)。在横纹肌肉瘤和9L-神经胶质瘤大鼠模型上评估了有无RT的ITPP的治疗效果。 ITPP在六个模型中增强了肿瘤氧合。每天一次2?g / kg ITPP,持续2?天,导致肿瘤复氧至少4?天。当在9L-神经胶质瘤上进行测试时,ITPP降低了六种细胞系的OCR,但对肿瘤灌注没有影响。 ITPP加RT不能改善横纹肌肉瘤的预后。在9L神经胶质瘤中,部分接受联合治疗的肿瘤已治愈,而其他肿瘤并未从治疗中受益。 ITPP在六个肿瘤模型中增加了氧合。 OCR降低可能有助于减少肿瘤缺氧。 RT与ITPP的结合对少数9L-神经胶质瘤有益,但在横纹肌肉瘤中则不存在。

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