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预测轴流生物反应器中多孔支架上HepG2细胞氧气和葡萄糖消耗的多种方法。

Multiple approaches to predicting oxygen and glucose consumptions by HepG2 cells on porous scaffolds in an axial-flow bioreactor.

作者信息

Podichetty Jagdeep T, Bhaskar Prasana R, Singarapu Kumar, Madihally Sundararajan V

机构信息

School of Chemical Engineering, Oklahoma State University, Stillwater, Oklahoma, 74078.

出版信息

Biotechnol Bioeng. 2015 Feb;112(2):393-404. doi: 10.1002/bit.25355. Epub 2014 Sep 26.

Abstract

In this study, the distribution of oxygen and glucose was evaluated along with consumption by hepatocytes using three different approaches. The methods include (i) Computational Fluid Dynamics (CFD) simulation, (ii) residence time distribution (RTD) analysis using a step-input coupled with segregation model or dispersion model, and (iii) experimentally determined consumption by HepG2 cells in an open-loop. Chitosan-gelatin (CG) scaffolds prepared by freeze-drying and polycaprolactone (PCL) scaffolds prepared by salt leaching technique were utilized for RTD analyses. The scaffold characteristics were used in CFD simulations i.e. Brinkman's equation for flow through porous medium, structural mechanics for fluid induced scaffold deformation, and advection-diffusion equation coupled with Michaelis-Menten rate equations for nutrient consumption. With the assumption that each hepatocyte behaves like a micro-batch reactor within the scaffold, segregation model was combined with RTD to determine exit concentration. A flow rate of 1 mL/min was used in the bioreactor seeded with 0.6 × 10(6) HepG2 cells/cm(3) on CG scaffolds and oxygen consumption was measured using two flow-through electrodes located at the inlet and outlet. Glucose in the spent growth medium was also analyzed. RTD results showed distribution of nutrients to depend on the surface characteristics of scaffolds. Comparisons of outlet oxygen concentrations between the simulation results, and experimental results showed good agreement with the dispersion model. Outlet oxygen concentrations from segregation model predictions were lower. Doubling the cell density showed a need for increasing the flow rate in CFD simulations. This integrated approach provide a useful strategy in designing bioreactors and monitoring tissue regeneration.

摘要

在本研究中,使用三种不同方法评估了肝细胞对氧气和葡萄糖的分布及其消耗情况。这些方法包括:(i)计算流体动力学(CFD)模拟;(ii)使用阶跃输入结合离析模型或扩散模型的停留时间分布(RTD)分析;以及(iii)通过开环实验测定HepG2细胞的消耗情况。通过冷冻干燥制备的壳聚糖 - 明胶(CG)支架和通过盐析技术制备的聚己内酯(PCL)支架用于RTD分析。支架特性用于CFD模拟,即用于流经多孔介质的布林克曼方程、用于流体诱导支架变形的结构力学,以及结合米氏速率方程用于营养物质消耗的平流 - 扩散方程。假设每个肝细胞在支架内的行为类似于微型间歇反应器,将离析模型与RTD相结合以确定出口浓度。在接种有0.6×10⁶个HepG2细胞/cm³的CG支架的生物反应器中使用1 mL/min的流速,并使用位于入口和出口的两个流通电极测量氧气消耗。还分析了用过的生长培养基中的葡萄糖。RTD结果表明营养物质的分布取决于支架的表面特性。模拟结果与实验结果之间出口氧气浓度的比较表明与扩散模型吻合良好。离析模型预测的出口氧气浓度较低。将细胞密度加倍表明在CFD模拟中需要提高流速。这种综合方法为设计生物反应器和监测组织再生提供了一种有用的策略。

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