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On a Minimal Model for Hemodynamics and Metabolism of Lactate: Application to Low Grade Glioma and Therapeutic Strategies

机译:乳酸血流动力学和代谢的最小模型:在低度胶质瘤和治疗策略中的应用

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WHO II low grade glioma evolves inevitably to anaplastic transformation. Magnetic resonance imaging is a good non-invasive way to watch it, by hemodynamic and metabolic modifications, thanks to multinuclear spectroscopy 1H/31P. In this work we study a multi-scale minimal model of hemodynamics and metabolism applied to the study of gliomas. This mathematical analysis leads us to a fast-slow system. The control of the position of the stationary point brings to the concept of domain of viability. Starting from this system, the equations bring to light the parameters that push glioma cells out of their domain of viability. Four fundamental factors are highlighted. The first two are cerebral blood flow and the rate of lactate transport through monocarboxylate transporters, which must be reduced in order to push glioma out of its domain of viability. Another factor is the intra arterial lactate, which must be increased. The last factor is pH, indeed a decrease of intra cellular pH could interfere with glioma growth. These reflections suggest that these four parameters could lead to new therapeutic strategies for the management of low grade gliomas.
机译:WHO II低度神经胶质瘤不可避免地演变为间变性。借助多核能谱1H / 31P,通过血流动力学和代谢改变,磁共振成像是一种很好的非侵入式观看方法。在这项工作中,我们研究了应用于神经胶质瘤研究的血液动力学和代谢的多尺度最小模型。这种数学分析使我们得到一个快速慢的系统。对固定点位置的控制带来了生存域的概念。从该系统开始,这些方程式揭示了将神经胶质瘤细胞推离其生存力域的参数。强调了四个基本因素。前两个是脑血流量和乳酸通过单羧酸盐转运蛋白的转运速率,必须降低这些速率才能将神经胶质瘤推出其生存能力。另一个因素是动脉内乳酸,必须增加。最后一个因素是pH,实际上细胞内pH的降低可能会干扰神经胶质瘤的生长。这些反映表明,这四个参数可以为治疗低度神经胶质瘤带来新的治疗策略。

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