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微载体培养中优化贴壁 MDCK 细胞数量分布的生长行为。

Growth behavior of number distributed adherent MDCK cells for optimization in microcarrier cultures.

机构信息

Max Planck Institute for Dynamics of Complex Technical Systems, Magdeburg, Sandtorstrasse 1, 39106 Magdeburg, Germany.

出版信息

Biotechnol Prog. 2009 Nov-Dec;25(6):1717-31. doi: 10.1002/btpr.262.

Abstract

An assay for measuring the number of adherent cells on microcarriers that is independent from dilution errors in sample preparation was used to investigate attachment dynamics and cell growth. It could be shown that the recovery of seeded cells is a function of the specific rates of cell attachment and cell death, and finally a function of the initial cell-to-bead ratio. An unstructured, segregated population balance model was developed that considers individual classes of microcarriers covered by 1-220 cells/bead. The model describes the distribution of initially attached cells and their growth in a microcarrier system. The model distinguishes between subpopulations of dividing and nondividing cells and describes in a detailed way cell attachment, cell growth, density-dependent growth inhibition, and basic metabolism of Madin-Darby canine kidney cells used in influenza vaccine manufacturing. To obtain a model approach that is suitable for process control applications, a reduced growth model without cell subpopulations, but with a formulation of the specific cell growth rate as a function of the initial cell distribution on microcarriers after seeding was developed. With both model approaches, the fraction of growth-inhibited cells could be predicted. Simulation results of two cultivations with a different number of initially seeded cells showed that the growth kinetics of adherent cells at the given cultivation conditions is mainly determined by the range of disparity in the initial distribution of cells on microcarriers after attachment.

摘要

一种用于测量微载体上贴壁细胞数量的测定方法,该方法独立于样品制备过程中的稀释误差,可以用于研究细胞的附着动力学和生长过程。结果表明,接种细胞的回收率是细胞附着和细胞死亡的特定速率的函数,最终是初始细胞-载体比的函数。建立了一个无结构的、分离的种群平衡模型,该模型考虑了被 1-220 个细胞/载体覆盖的单个微载体类别。该模型描述了微载体系统中初始附着细胞的分布及其生长情况。该模型区分了分裂和非分裂细胞的亚群,并详细描述了用于流感疫苗生产的 Madin-Darby 犬肾细胞的细胞附着、细胞生长、密度依赖性生长抑制以及基本代谢。为了获得适合过程控制应用的模型方法,开发了一种没有细胞亚群的简化生长模型,但将特定细胞生长速率的公式表述为接种后微载体上初始细胞分布的函数。通过这两种模型方法,可以预测生长受抑制细胞的分数。两种接种不同初始细胞数的培养的模拟结果表明,在给定的培养条件下,贴壁细胞的生长动力学主要由附着后微载体上细胞初始分布的差异范围决定。

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