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走向癌症的伊辛模型及其他。

Toward an Ising model of cancer and beyond.

机构信息

Department of Chemistry, Princeton University, Princeton, NJ 08544, USA.

出版信息

Phys Biol. 2011 Feb;8(1):015017. doi: 10.1088/1478-3975/8/1/015017. Epub 2011 Feb 7.

Abstract

The holy grail of tumor modeling is to formulate theoretical and computational tools that can be utilized in the clinic to predict neoplastic progression and propose individualized optimal treatment strategies to control cancer growth. In order to develop such a predictive model, one must account for the numerous complex mechanisms involved in tumor growth. Here we review the research work that we have done toward the development of an 'Ising model' of cancer. The Ising model is an idealized statistical-mechanical model of ferromagnetism that is based on simple local-interaction rules, but nonetheless leads to basic insights and features of real magnets, such as phase transitions with a critical point. The review begins with a description of a minimalist four-dimensional (three dimensions in space and one in time) cellular automaton (CA) model of cancer in which cells transition between states (proliferative, hypoxic and necrotic) according to simple local rules and their present states, which can viewed as a stripped-down Ising model of cancer. This model is applied to study the growth of glioblastoma multiforme, the most malignant of brain cancers. This is followed by a discussion of the extension of the model to study the effect on the tumor dynamics and geometry of a mutated subpopulation. A discussion of how tumor growth is affected by chemotherapeutic treatment, including induced resistance, is then described. We then describe how to incorporate angiogenesis as well as the heterogeneous and confined environment in which a tumor grows in the CA model. The characterization of the level of organization of the invasive network around a solid tumor using spanning trees is subsequently discussed. Then, we describe open problems and future promising avenues for future research, including the need to develop better molecular-based models that incorporate the true heterogeneous environment over wide range of length and time scales (via imaging data), cell motility, oncogenes, tumor suppressor genes and cell-cell communication. A discussion about the need to bring to bear the powerful machinery of the theory of heterogeneous media to better understand the behavior of cancer in its microenvironment is presented. Finally, we propose the possibility of using optimization techniques, which have been used profitably to understand physical phenomena, in order to devise therapeutic (chemotherapy/radiation) strategies and to understand tumorigenesis itself.

摘要

肿瘤建模的圣杯是制定可用于临床的理论和计算工具,以预测肿瘤进展并提出个体化的最佳治疗策略来控制癌症生长。为了开发这样的预测模型,必须考虑到肿瘤生长中涉及的许多复杂机制。在这里,我们回顾了我们在开发癌症“伊辛模型”方面所做的研究工作。伊辛模型是铁磁体的理想化统计力学模型,基于简单的局部相互作用规则,但仍能得出真实磁铁的基本见解和特征,例如具有临界点的相变。综述首先描述了一个最小的四维(三维空间和一维时间)细胞自动机(CA)癌症模型,其中细胞根据简单的局部规则和它们的当前状态在状态(增殖、缺氧和坏死)之间转换,可以看作是癌症的简化伊辛模型。该模型应用于研究多形性胶质母细胞瘤的生长,这是最恶性的脑癌。接下来讨论了将模型扩展到研究突变亚群对肿瘤动力学和几何形状的影响。然后描述了化疗治疗如何影响肿瘤生长,包括诱导耐药性。接下来描述了如何在 CA 模型中纳入血管生成以及肿瘤生长的异质和受限环境。随后讨论了使用生成树来描述实体瘤周围侵袭网络的组织水平。然后,我们描述了未来研究的开放性问题和有前途的途径,包括需要开发更好的基于分子的模型,这些模型可以在广泛的长度和时间尺度(通过成像数据)内纳入真实的异质环境、细胞迁移、癌基因、肿瘤抑制基因和细胞间通讯。提出了利用非均匀介质理论的强大机制来更好地理解癌症在其微环境中的行为的必要性。最后,我们提出了使用优化技术的可能性,这些技术已经被用于理解物理现象,以便设计治疗(化疗/放疗)策略并了解肿瘤发生本身。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2974/3151151/ff5076399973/nihms308329f1.jpg

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