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一种简单且准确的基于规则的建模框架,用于在二维培养中模拟L1CAM对胶质母细胞瘤细胞运动性和增殖的自分泌/旁分泌刺激。

A simple and accurate rule-based modeling framework for simulation of autocrine/paracrine stimulation of glioblastoma cell motility and proliferation by L1CAM in 2-D culture.

作者信息

Caccavale Justin, Fiumara David, Stapf Michael, Sweitzer Liedeke, Anderson Hannah J, Gorky Jonathan, Dhurjati Prasad, Galileo Deni S

机构信息

Department of Chemical and Biomolecular Engineering, University of Delaware, Newark, DE, 19716, USA.

Department of Mathematical Sciences, University of Delaware, Newark, DE, 19716, USA.

出版信息

BMC Syst Biol. 2017 Dec 11;11(1):124. doi: 10.1186/s12918-017-0516-z.

Abstract

BACKGROUND

Glioblastoma multiforme (GBM) is a devastating brain cancer for which there is no known cure. Its malignancy is due to rapid cell division along with high motility and invasiveness of cells into the brain tissue. Simple 2-dimensional laboratory assays (e.g., a scratch assay) commonly are used to measure the effects of various experimental perturbations, such as treatment with chemical inhibitors. Several mathematical models have been developed to aid the understanding of the motile behavior and proliferation of GBM cells. However, many are mathematically complicated, look at multiple interdependent phenomena, and/or use modeling software not freely available to the research community. These attributes make the adoption of models and simulations of even simple 2-dimensional cell behavior an uncommon practice by cancer cell biologists.

RESULTS

Herein, we developed an accurate, yet simple, rule-based modeling framework to describe the in vitro behavior of GBM cells that are stimulated by the L1CAM protein using freely available NetLogo software. In our model L1CAM is released by cells to act through two cell surface receptors and a point of signaling convergence to increase cell motility and proliferation. A simple graphical interface is provided so that changes can be made easily to several parameters controlling cell behavior, and behavior of the cells is viewed both pictorially and with dedicated graphs. We fully describe the hierarchical rule-based modeling framework, show simulation results under several settings, describe the accuracy compared to experimental data, and discuss the potential usefulness for predicting future experimental outcomes and for use as a teaching tool for cell biology students.

CONCLUSIONS

It is concluded that this simple modeling framework and its simulations accurately reflect much of the GBM cell motility behavior observed experimentally in vitro in the laboratory. Our framework can be modified easily to suit the needs of investigators interested in other similar intrinsic or extrinsic stimuli that influence cancer or other cell behavior. This modeling framework of a commonly used experimental motility assay (scratch assay) should be useful to both researchers of cell motility and students in a cell biology teaching laboratory.

摘要

背景

多形性胶质母细胞瘤(GBM)是一种毁灭性的脑癌,目前尚无已知的治愈方法。其恶性程度归因于细胞的快速分裂以及细胞向脑组织的高迁移率和侵袭性。简单的二维实验室检测方法(例如划痕试验)通常用于测量各种实验干扰的影响,如用化学抑制剂进行处理。已经开发了几种数学模型来帮助理解GBM细胞的运动行为和增殖。然而,许多模型在数学上很复杂,研究多个相互依赖的现象,和/或使用研究界无法免费获得的建模软件。这些特性使得即使是简单的二维细胞行为的模型和模拟在癌细胞生物学家中也不常被采用。

结果

在此,我们开发了一个准确但简单的基于规则的建模框架,以使用免费的NetLogo软件描述受L1CAM蛋白刺激的GBM细胞的体外行为。在我们的模型中,L1CAM由细胞释放,通过两种细胞表面受体和一个信号汇聚点起作用,以增加细胞运动性和增殖。提供了一个简单的图形界面,以便可以轻松更改控制细胞行为的几个参数,并以图形方式和专用图表查看细胞行为。我们全面描述了基于规则的分层建模框架,展示了几种设置下的模拟结果,描述了与实验数据相比的准确性,并讨论了预测未来实验结果以及用作细胞生物学学生教学工具的潜在用途。

结论

得出的结论是,这个简单的建模框架及其模拟准确地反映了在实验室体外实验中观察到的许多GBM细胞运动行为。我们的框架可以轻松修改,以满足对影响癌症或其他细胞行为的其他类似内在或外在刺激感兴趣的研究人员的需求。这种常用实验运动检测方法(划痕试验)的建模框架对细胞运动研究人员和细胞生物学教学实验室的学生都应该有用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/16b5/5725844/003e9228884b/12918_2017_516_Fig1_HTML.jpg

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