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静态条件下同型细胞聚集动力学模型。

A model for the kinetics of homotypic cellular aggregation under static conditions.

作者信息

Neelamegham S, Munn L L, Zygourakis K

机构信息

Department of Chemical Engineering, Rice University, Houston, Texas 77251-1892, USA.

出版信息

Biophys J. 1997 Jan;72(1):51-64. doi: 10.1016/S0006-3495(97)78646-6.

Abstract

We present the formulation and testing of a mathematical model for the kinetics of homotypic cellular aggregation. The model considers cellular aggregation under no-flow conditions as a two-step process. Individual cells and cell aggregates 1) move on the tissue culture surface and 2) collide with other cells (or aggregates). These collisions lead to the formation of intercellular bonds. The aggregation kinetics are described by a system of coupled, nonlinear ordinary differential equations, and the collision frequency kernel is derived by extending Smoluchowski's colloidal flocculation theory to cell migration and aggregation on a two-dimensional surface. Our results indicate that aggregation rates strongly depend upon the motility of cells and cell aggregates, the frequency of cell-cell collisions, and the strength of intercellular bonds. Model predictions agree well with data from homotypic lymphocyte aggregation experiments using Jurkat cells activated by 33B6, an antibody to the beta 1 integrin. Since cell migration speeds and all the other model parameters can be independently measured, the aggregation model provides a quantitative methodology by which we can accurately evaluate the adhesivity and aggregation behavior of cells.

摘要

我们提出了一种用于同型细胞聚集动力学的数学模型的公式化表述及测试。该模型将无流动条件下的细胞聚集视为一个两步过程。单个细胞和细胞聚集体:1)在组织培养表面移动,2)与其他细胞(或聚集体)碰撞。这些碰撞导致细胞间键的形成。聚集动力学由一组耦合的非线性常微分方程系统描述,并且通过将斯莫卢霍夫斯基的胶体絮凝理论扩展到二维表面上的细胞迁移和聚集来推导碰撞频率核。我们的结果表明,聚集速率强烈依赖于细胞和细胞聚集体的运动性、细胞 - 细胞碰撞的频率以及细胞间键的强度。模型预测与使用由β1整合素抗体33B6激活的Jurkat细胞进行的同型淋巴细胞聚集实验的数据吻合良好。由于细胞迁移速度和所有其他模型参数都可以独立测量,因此聚集模型提供了一种定量方法,通过该方法我们可以准确评估细胞的粘附性和聚集行为。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/efcb/1184296/5e9c4a275293/biophysj00039-0054-a.jpg

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