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首页> 外文期刊>Journal of magnetic resonance imaging: JMRI >Intracellular pH measured by 31 31 P‐MR‐spectroscopy might predict site of progression in recurrent glioblastoma under antiangiogenic therapy
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Intracellular pH measured by 31 31 P‐MR‐spectroscopy might predict site of progression in recurrent glioblastoma under antiangiogenic therapy

机译:通过311111111111111111113测量的细胞内pH可以预测抗血管生成治疗下复发胶质母细胞瘤的进展部位

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摘要

Purpose In solid tumors, changes in the expression/activity of plasma membrane ion transporters facilitate proton efflux and enable tumor cells to maintain a higher intracellular pH (pH i ), while the microenvironment (pH e ) is commonly more acidic. This supports various tumor‐promoting mechanisms. We propose that these changes in pH take place before a magnetic resonance imaging (MRI)‐detectable brain tumor recurrence occurs. Materials and Methods We enrolled 66 patients with recurrent glioblastoma, treated with bevacizumab. Patients received a baseline and 8‐week follow‐up MRI including 1 H/ 31 P MRSI (spectroscopy) on a 3T clinical scanner, until progressive disease according to Response Assessment in Neuro‐Oncology (RANO) criteria occurred. Fourteen patients showed a distant or diffuse tumor recurrence (subsequent tumor) during treatment and were therefore selected for further evaluation. At the site of the subsequent tumor, an area of interest for MRSI voxel selection was retrospectively defined on radiographically unaffected baseline MRI sequences. Results Before treatment, pH i in the area of interest (subsequent tumor) was significantly higher than pH i of the contralateral normal‐appearing tissue (control; P ??0.001). It decreased at the time of best response ( P ?=?0.06), followed by a significant increase at progression ( P ?=?0.03; baseline mean: 7.06, median: 7.068, SD: 0.032; best response mean: 7.044, median: 7.036, SD: 0.025; progression mean: 7.08, median: 7.095, SD 0.035). Until progression, the subsequent tumor was not detectable on standard MRI sequences. The area of existing tumor responded similar, but changes were not significant (decrease P ?=?0.22; increase P ?=?0.28). Conclusion Elevated pH i in radiographically unaffected tissue at baseline might precede MRI‐detectable progression in patients with recurrent glioblastoma treated with bevacizumab. Level of Evidence: 2 Technical Efficacy: Stage 3 J. Magn. Reson. Imaging 2017;46:1200–1208.
机译:在实体肿瘤中的目的,血浆膜离子转运蛋白的表达/活性的变化促进质子流出并使肿瘤细胞保持更高的细胞内pH(pH I),而微环境(pHe)通常更酸性。这支持各种肿瘤促进机制。我们提出在磁共振成像(MRI) - 可伸展的脑肿瘤复发之前进行的这些改变发生。我们注册了66例复制胶质母细胞瘤的材料和方法,用贝伐单抗治疗。患者接受了基线和8周的后续MRI,包括3T临床扫描仪的1 H / 31 p MRSI(光谱学),直到根据神经肿瘤学的反应评估(RANO)标准发生渐进疾病。在治疗期间,十四名患者展示了遥远或弥漫性肿瘤复发(随后的肿瘤),因此选择进一步评估。在随后的肿瘤部位,在射线照射非受影响的基线MRI序列上回顾性地定义了MRSI体素选择的感兴趣区域。结果在治疗前,感兴趣区域(随后肿瘤)的pH I显着高于对侧正常出现组织的pH(对照;p≤≤0.001)。它在最佳反应时减少(p?= 0.06),然后在进展情况下显着增加(p?= 0.03;基线平均值:7.06,中位数:7.068,SD:0.032;最佳响应意味着:7.044,中位数:7.036,SD:0.025;进展均值:7.08,中位数:7.095,SD 0.035)。直到进展,在标准MRI序列上未检测到随后的肿瘤。现有肿瘤的面积相似,但变化不显着(减少p?= 0.22;增加p?= 0.28)。结论在基线上射线照射的组织中的pH I升高,可能在用Bevacizumab处理的复发性胶质母细胞瘤患者之前先发制MRI可检测的进展。证据水平:2技术疗效:第3阶段J. MANG。恢复。 2017年成像; 46:1200-1208。

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