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Methods for improving simulations of biological systems: systemic computation and fractal proteins

机译:改善生物系统模拟的方法:系统计算和分形蛋白

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摘要

Modelling and simulation are becoming essential for new fields such as synthetic biology. Perhaps the most important aspect of modelling is to follow a clear design methodology that will help to highlight unwanted deficiencies. The use of tools designed to aid the modelling process can be of benefit in many situations. In this paper, the modelling approach called systemic computation (SC) is introduced. SC is an interaction-based language, which enables individual-based expression and modelling of biological systems, and the interactions between them. SC permits a precise description of a hypothetical mechanism to be written using an intuitive graph-based or a calculus-based notation. The same description can then be directly run as a simulation, merging the hypothetical mechanism and the simulation into the same entity. However, even when using well-designed modelling tools to produce good models, the best model is not always the most accurate one. Frequently, computational constraints or lack of data make it infeasible to model an aspect of biology. Simplification may provide one way forward, but with inevitable consequences of decreased accuracy. Instead of attempting to replace an element with a simpler approximation, it is sometimes possible to substitute the element with a different but functionally similar component. In the second part of this paper, this modelling approach is described and its advantages are summarized using an exemplar: the fractal protein model. Finally, the paper ends with a discussion of good biological modelling practice by presenting lessons learned from the use of SC and the fractal protein model.
机译:对于诸如合成生物学之类的新领域,建模和仿真变得至关重要。建模最重要的方面也许是遵循清晰的设计方法,这将有助于突出不必要的缺陷。在许多情况下,使用旨在辅助建模过程的工具可能会有所帮助。本文介绍了一种称为系统计算(SC)的建模方法。 SC是一种基于交互的语言,它使基于生物系统的个体表达和建模以及它们之间的交互成为可能。 SC允许使用直观的基于图形或基于演算的表示法来编写假设机制的精确描述。然后,可以将相同的描述直接作为模拟运行,将假设机制和模拟合并到同一实体中。但是,即使使用精心设计的建模工具生成好的模型,最佳模型也不总是最准确的模型。通常,计算上的限制或缺乏数据使得对生物学的一个方面进行建模是不可行的。简化可以提供一种前进的方向,但是不可避免地会降低准确性。代替尝试用更简单的近似替换元素,有时可以用不同但功能相似的组件替换元素。在本文的第二部分中,将描述这种建模方法,并使用一个示例:分形蛋白质模型来总结其优势。最后,本文通过介绍从使用SC和分形蛋白模型中学到的经验教训,讨论了良好的生物学建模实践。

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