首页> 美国卫生研究院文献>Tissue Engineering. Part C Methods >Effect of Oxygen Concentration on Viability and Metabolism in a Fluidized-Bed Bioartificial Liver Using 31P and 13C NMR Spectroscopy
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Effect of Oxygen Concentration on Viability and Metabolism in a Fluidized-Bed Bioartificial Liver Using 31P and 13C NMR Spectroscopy

机译:使用31P和13C NMR光谱分析流化床生物人工肝中氧气浓度对活力和代谢的影响

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摘要

Many oxygen mass-transfer modeling studies have been performed for various bioartificial liver (BAL) encapsulation types; yet, to our knowledge, there is no experimental study that directly and noninvasively measures viability and metabolism as a function of time and oxygen concentration. We report the effect of oxygen concentration on viability and metabolism in a fluidized-bed NMR-compatible BAL using in vivo 31P and 13C NMR spectroscopy, respectively, by monitoring nucleotide triphosphate (NTP) and 13C-labeled nutrient metabolites, respectively. Fluidized-bed bioreactors eliminate the potential channeling that occurs with packed-bed bioreactors and serve as an ideal experimental model for homogeneous oxygen distribution. Hepatocytes were electrostatically encapsulated in alginate (avg. diameter, 500 μm; 3.5×107 cells/mL) and perfused at 3 mL/min in a 9-cm (inner diameter) cylindrical glass NMR tube. Four oxygen treatments were tested and validated by an in-line oxygen electrode: (1) 95:5 oxygen:carbon dioxide (carbogen), (2) 75:20:5 nitrogen:oxygen:carbon dioxide, (3) 60:35:5 nitrogen:oxygen:carbon dioxide, and (4) 45:50:5 nitrogen:oxygen:carbon dioxide. With 20% oxygen, β-NTP steadily decreased until it was no longer detected at 11 h. The 35%, 50%, and 95% oxygen treatments resulted in steady β-NTP levels throughout the 28-h experimental period. For the 50% and 95% oxygen treatment, a 13C NMR time course (∼5 h) revealed 2-13C-glycine and 2-13C-glucose to be incorporated into [2-13C-glycyl]glutathione (GSH) and 2-13C-lactate, respectively, with 95% having a lower rate of lactate formation. 31P and 13C NMR spectroscopy is a noninvasive method for determining viability and metabolic rates. Modifying tissue-engineered devices to be NMR compatible is a relatively easy and inexpensive process depending on the bioreactor shape.
机译:对于各种生物人工肝(BAL)封装类型,已经进行了许多氧气传质建模研究。然而,据我们所知,尚无任何实验研究能够直接和无创地测量生存力和新陈代谢随时间和氧气浓度的变化。我们通过监测核苷酸分别报道了体内 31 P和 13 C NMR光谱法分析氧浓度对流化床NMR兼容BAL中活力和代谢的影响三磷酸(NTP)和 13 C标记的营养代谢产物。流化床生物反应器消除了填充床生物反应器可能发生的窜流,并且是均匀分布氧气的理想实验模型。将肝细胞静电包封在藻酸盐(平均直径500μm; 3.5×10 7个细胞/ mL)中,并以3μmL/ min的速度在9厘米(内径)圆柱形玻璃NMR管中灌注。通过串联的氧气电极测试并验证了四种氧气处理方法:(1)95:5氧气:二氧化碳(碳源),(2)75:20:5氮气:氧气:二氧化碳,(3)60:35 :5氮气:氧气:二氧化碳,和(4)45:50:5氮气:氧气:二氧化碳。在氧气含量为20%的情况下,β-NTP逐渐降低,直到在11 h不再被检测到。 35%,50%和95%的氧气处理在整个28小时的实验期内均产生稳定的β-NTP水平。对于50%和95%的氧气处理, 13 C NMR时程(〜5 h)显示2- 13 C-甘氨酸和2- 13 < / sup> C-葡萄糖分别掺入[2- 13 C-甘氨酰]谷胱甘肽(GSH)和2- 13 C-乳酸酯中,其中95%具有乳酸形成率较低。 31 P和 13 C NMR光谱法是一种测定生存力和代谢率的非侵入性方法。根据生物反应器的形状,将组织工程设备修改为与NMR兼容是一个相对简单且便宜的过程。

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