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开发一个三维多尺度人类表皮计算模型。

Development of a three dimensional multiscale computational model of the human epidermis.

机构信息

Department of Computer Science, University of Sheffield, Sheffield, United Kingdom.

出版信息

PLoS One. 2010 Jan 14;5(1):e8511. doi: 10.1371/journal.pone.0008511.

Abstract

Transforming Growth Factor (TGF-beta1) is a member of the TGF-beta superfamily ligand-receptor network. and plays a crucial role in tissue regeneration. The extensive in vitro and in vivo experimental literature describing its actions nevertheless describe an apparent paradox in that during re-epithelialisation it acts as proliferation inhibitor for keratinocytes. The majority of biological models focus on certain aspects of TGF-beta1 behaviour and no one model provides a comprehensive story of this regulatory factor's action. Accordingly our aim was to develop a computational model to act as a complementary approach to improve our understanding of TGF-beta1. In our previous study, an agent-based model of keratinocyte colony formation in 2D culture was developed. In this study this model was extensively developed into a three dimensional multiscale model of the human epidermis which is comprised of three interacting and integrated layers: (1) an agent-based model which captures the biological rules governing the cells in the human epidermis at the cellular level and includes the rules for injury induced emergent behaviours, (2) a COmplex PAthway SImulator (COPASI) model which simulates the expression and signalling of TGF-beta1 at the sub-cellular level and (3) a mechanical layer embodied by a numerical physical solver responsible for resolving the forces exerted between cells at the multi-cellular level. The integrated model was initially validated by using it to grow a piece of virtual epidermis in 3D and comparing the in virtuo simulations of keratinocyte behaviour and of TGF-beta1 signalling with the extensive research literature describing this key regulatory protein. This research reinforces the idea that computational modelling can be an effective additional tool to aid our understanding of complex systems. In the accompanying paper the model is used to explore hypotheses of the functions of TGF-beta1 at the cellular and subcellular level on different keratinocyte populations during epidermal wound healing.

摘要

转化生长因子(TGF-β1)是 TGF-β 超家族配体-受体网络的成员,在组织再生中起着至关重要的作用。尽管大量描述其作用的体外和体内实验文献描述了一个明显的悖论,即在再上皮化过程中,它作为角质形成细胞的增殖抑制剂。大多数生物模型都集中在 TGF-β1 行为的某些方面,没有一个模型提供了这个调节因子作用的全面描述。因此,我们的目标是开发一个计算模型,作为一种补充方法来提高我们对 TGF-β1 的理解。在我们之前的研究中,开发了一个二维培养角质形成细胞集落形成的基于代理的模型。在这项研究中,这个模型被广泛地发展成为一个三维多层次的人类表皮模型,它由三个相互作用和集成的层组成:(1)一个基于代理的模型,捕获了在细胞水平上控制人类表皮细胞的生物学规则,包括损伤诱导的新兴行为的规则,(2)一个 COmplex PAthway SImulator(COPASI)模型,模拟 TGF-β1 在亚细胞水平上的表达和信号传递,(3)一个由负责解决多细胞水平细胞间力的数值物理求解器体现的机械层。该集成模型最初通过使用它在 3D 中生长一块虚拟表皮并将角质形成细胞行为和 TGF-β1 信号的虚拟模拟与描述这种关键调节蛋白的广泛研究文献进行比较来进行验证。这项研究加强了这样一种观点,即计算建模可以是一种有效的附加工具,有助于我们理解复杂系统。在随附的论文中,该模型被用于探索在表皮伤口愈合过程中,TGF-β1 在不同角质形成细胞群体中的细胞和亚细胞水平上的功能假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f5d/2799518/993bd5ac7f5e/pone.0008511.g001.jpg

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