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对两种具有广泛不同比例放射生物学缺氧细胞的小鼠肿瘤细胞系进行体内³¹P核磁共振波谱分析。

31P NMR spectroscopy in vivo of two murine tumor lines with widely different fractions of radiobiologically hypoxic cells.

作者信息

Rofstad E K, Howell R L, DeMuth P, Ceckler T L, Sutherland R M

机构信息

Experimental Therapeutics Division, University of Rochester Cancer Center, New York 14642.

出版信息

Int J Radiat Biol. 1988 Oct;54(4):635-49. doi: 10.1080/09553008814552071.

Abstract

Energy and lipid metabolism as well as tumor pH in two murine tumor lines, the KHT and RIF-1 sarcomas, were studied using 31P NMR spectroscopy. Possible relationships between spectral parameters on the one hand and volume fraction of necrosis and fraction of radiobiologically hypoxic cells on the other were investigated. For both tumor lines the PCr and NTP beta resonances decreased and the Pi resonance increased significantly with increasing tumor volume in the volume range 100-4000 mm3. This decrease in bioenergetic status was accompanied by a decrease in tumor pH from about 7.2 to about 6.8. The NTP beta resonance and the tumor pH tended to be somewhat higher and the Pi resonance somewhat lower for the KHT than for the RIF-1 tumors. Linear relationships were found between tumor pH and Pi or (PCr + NTP beta)/Pi for both tumor lines (P much less than 0.05). The PME resonance increased slightly and the PDE resonance decreased slightly during tumor growth and were not significantly different for the KHT and the RIF-1 tumors. The volume fraction of necrosis was about 5 per cent in both lines at a tumor volume of 100 mm3 and increased to about 30 per cent (KHT) and 50 per cent (RIF-1) at a tumor volume of 4000 mm3. The fraction of radiobiologically hypoxic cells was found to increase from 12 to 23 per cent for the KHT line and from 0.9 to 1.7 per cent for the RIF-1 line when tumor volume was increased from about 200 to about 2000 mm3. The volume-dependence of the 31P NMR spectral parameters indicated increased nutritional deprivation and development of hypoxia and necrosis during tumor growth, and was thus qualitatively in good agreement with the changes observed in necrotic and hypoxic fraction. However, quantitative relationships between any spectral parameter and necrotic or hypoxic fraction across tumor lines were not found, implying that other physiological parameters and/or cellular characteristics may contribute significantly to a 31P NMR tumor spectrum. Consequently, 31P NMR spectra of untreated tumors have to be supplemented with other tumor data, e.g. rate of oxygen consumption, cell survival time under hypoxic stress and/or fraction of metabolically active, non-clonogenic hypoxic cells, to be useful in quantitative determination of tumor hypoxia and hence prediction of tumor radioresistance caused by hypoxia.

摘要

利用31P核磁共振波谱研究了两种小鼠肿瘤模型,即KHT和RIF-1肉瘤的能量与脂质代谢以及肿瘤pH值。研究了一方面光谱参数与另一方面坏死体积分数和放射生物学低氧细胞分数之间的可能关系。对于这两种肿瘤模型,在100 - 4000 mm3的体积范围内,随着肿瘤体积增加,磷酸肌酸(PCr)和NTPβ共振降低,无机磷酸(Pi)共振显著增加。生物能量状态的这种降低伴随着肿瘤pH值从约7.2降至约6.8。KHT肿瘤的NTPβ共振和肿瘤pH值往往略高于RIF-1肿瘤,而Pi共振则略低于RIF-1肿瘤。发现两种肿瘤模型的肿瘤pH值与Pi或(PCr + NTPβ)/Pi之间均存在线性关系(P远小于0.05)。在肿瘤生长过程中,磷酸单酯(PME)共振略有增加,磷酸二酯(PDE)共振略有降低,KHT和RIF-1肿瘤之间无显著差异。在肿瘤体积为100 mm3时,两种肿瘤模型的坏死体积分数均约为5%,在肿瘤体积为4000 mm3时,分别增加至约30%(KHT)和50%(RIF-1)。当肿瘤体积从约200 mm3增加至约2000 mm3时,发现KHT肿瘤模型的放射生物学低氧细胞分数从12%增加至23%,RIF-1肿瘤模型从0.9%增加至1.7%。31P核磁共振波谱参数的体积依赖性表明,在肿瘤生长过程中营养剥夺增加,缺氧和坏死情况加剧,因此在定性上与坏死和低氧分数的变化良好吻合。然而,未发现跨肿瘤模型的任何光谱参数与坏死或低氧分数之间的定量关系,这意味着其他生理参数和/或细胞特征可能对31P核磁共振肿瘤谱有显著贡献。因此,未经处理的肿瘤的31P核磁共振波谱必须辅以其他肿瘤数据,例如耗氧率、低氧应激下的细胞存活时间和/或代谢活跃的非克隆性低氧细胞分数,才能用于定量测定肿瘤低氧情况,进而预测由低氧引起的肿瘤放射抗性。

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