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活体人乳腺癌细胞中高极化13C1-丙酮酸转运与代谢的动力学

Kinetics of hyperpolarized 13C1-pyruvate transport and metabolism in living human breast cancer cells.

作者信息

Harris Talia, Eliyahu Galit, Frydman Lucio, Degani Hadassa

机构信息

Department of Chemical Physics, Weizmann Institute, Rehovot 76100, Israel.

出版信息

Proc Natl Acad Sci U S A. 2009 Oct 27;106(43):18131-6. doi: 10.1073/pnas.0909049106. Epub 2009 Oct 13.

Abstract

Metabolic fluxes can serve as specific biomarkers for detecting malignant transformations, tumor progression, and response to microenvironmental changes and treatment procedures. We present noninvasive hyperpolarized (13)C NMR investigations on the metabolic flux of pyruvate to lactate, in a well-controlled injection/perfusion system using T47D human breast cancer cells. Initial rates of pyruvate-to-lactate conversion were obtained by fitting the hyperpolarized (13)C and ancillary (31)P NMR data to a model, yielding both kinetic parameters and mechanistic insight into this conversion. Transport was found to be the rate-limiting process for the conversion of extracellular pyruvate to lactate with K(m) = 2.14 +/- 0.03 mM, typical of the monocarboxylate transporter 1 (MCT1), and a V(max) = 27.6 +/- 1.1 fmolxmin(-1).cell(-1), in agreement with the high expression level of this transporter. Modulation of the environment to hypoxic conditions as well as suppression of cells' perfusion enhanced the rate of pyruvate-to-lactate conversion, presumably by up-regulation of the MCT1. Conversely, the addition of quercetin, a flavonoidal MCT1 inhibitor, markedly reduces the apparent rate of pyruvate-to-lactate conversion. These results suggest that hyperpolarized (13)C(1)-pyruvate may be a useful magnetic resonance biomarker of MCT regulation and malignant transformations in breast cancer.

摘要

代谢通量可作为检测恶性转化、肿瘤进展以及对微环境变化和治疗程序反应的特定生物标志物。我们在一个使用T47D人乳腺癌细胞的严格控制的注射/灌注系统中,对丙酮酸向乳酸的代谢通量进行了非侵入性超极化(13)C核磁共振研究。通过将超极化(13)C和辅助(31)P核磁共振数据拟合到一个模型中,获得了丙酮酸向乳酸转化的初始速率,从而得到了动力学参数以及对这种转化的机制性见解。发现转运是细胞外丙酮酸转化为乳酸的限速过程,其米氏常数(K(m))=2.14±0.03 mM,这是单羧酸转运蛋白1(MCT1)的典型值,最大反应速率(V(max))=27.6±1.1 fmol·min(-1)·cell(-1),这与该转运蛋白的高表达水平一致。将环境调节为缺氧条件以及抑制细胞灌注可提高丙酮酸向乳酸的转化速率,推测这是通过上调MCT1实现的。相反,添加黄酮类MCT1抑制剂槲皮素可显著降低丙酮酸向乳酸转化的表观速率。这些结果表明,超极化(13)C(1)-丙酮酸可能是乳腺癌中MCT调节和恶性转化的一种有用的磁共振生物标志物。

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