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通过 13C 磁共振波谱技术检测肿瘤对血管破坏剂的反应。

Detection of tumor response to a vascular disrupting agent by hyperpolarized 13C magnetic resonance spectroscopy.

机构信息

Department of Biochemistry, University of Cambridge, Cambridge, UK.

出版信息

Mol Cancer Ther. 2010 Dec;9(12):3278-88. doi: 10.1158/1535-7163.MCT-10-0706.

Abstract

Nuclear spin hyperpolarization can dramatically increase the sensitivity of the (13)C magnetic resonance experiment, allowing dynamic measurements of the metabolism of hyperpolarized (13)C-labeled substrates in vivo. Here, we report a preclinical study of the response of lymphoma tumors to the vascular disrupting agent (VDA), combretastatin-A4-phosphate (CA4P), as detected by measuring changes in tumor metabolism of hyperpolarized [1-(13)C]pyruvate and [1,4-(13)C(2)]fumarate. These measurements were compared with dynamic contrast agent-enhanced magnetic resonance imaging (DCE-MRI) measurements of tumor vascular function and diffusion-weighted MRI (DW-MRI) measurements of the tumor cell necrosis that resulted from subsequent loss of tumor perfusion. The rate constant describing flux of hyperpolarized (13)C label between [1-(13)C]pyruvate and lactate was decreased by 34% within 6 hours of CA4P treatment and remained at this lower level at 24 hours. The rate constant describing production of labeled malate from hyperpolarized [1,4-(13)C(2)]fumarate increased 1.6-fold and 2.5-fold at 6 and 24 hours after treatment, respectively, and correlated with the degree of necrosis detected in histologic sections. Although DCE-MRI measurements showed a substantial reduction in perfusion at 6 hours after treatment, which had recovered by 24 hours, DW-MRI showed no change in the apparent diffusion coefficient of tumor water at 6 hours after treatment, although there was a 32% increase at 24 hours (P < 0.02) when regions of extensive necrosis were observed by histology. Measurements of hyperpolarized [1-(13)C]pyruvate and [1,4-(13)C(2)]fumarate metabolism may provide, therefore, a more sustained and sensitive indicator of response to a VDA than DCE-MRI or DW-MRI, respectively.

摘要

核自旋超极化能极大地提高 (13)C 磁共振实验的灵敏度,从而可以动态测量活体中 (13)C 标记的底物的代谢。在这里,我们报告了一项关于淋巴瘤肿瘤对血管破坏剂(VDA),combretastatin-A4-磷酸(CA4P)的反应的临床前研究,该研究通过测量极化 [1-(13)C]丙酮酸和 [1,4-(13)C(2)]富马酸的肿瘤代谢变化来检测。这些测量结果与肿瘤血管功能的动态对比剂增强磁共振成像(DCE-MRI)测量结果和随后肿瘤灌注丧失导致的肿瘤细胞坏死的弥散加权磁共振成像(DW-MRI)测量结果进行了比较。描述 [1-(13)C]丙酮酸和乳酸之间的极化(13)C 标记物通量的速率常数在 CA4P 处理后 6 小时内降低了 34%,并在 24 小时内保持在较低水平。描述从极化 [1,4-(13)C(2)]富马酸产生标记物苹果酸的速率常数在治疗后 6 小时和 24 小时分别增加了 1.6 倍和 2.5 倍,并且与组织学切片中检测到的坏死程度相关。尽管 DCE-MRI 测量结果显示治疗后 6 小时灌注明显减少,但在 24 小时后已恢复,但 DW-MRI 治疗后 6 小时肿瘤水的表观扩散系数没有变化,尽管组织学观察到广泛坏死区域时增加了 32%(P <0.02)。因此,与 DCE-MRI 或 DW-MRI 相比,极化 [1-(13)C]丙酮酸和 [1,4-(13)C(2)]富马酸代谢的测量可能提供了对 VDA 反应的更持续和敏感的指标。

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