Covid-19病毒的分割马尔可夫模型

4open Pub Date : 2020-01-01 DOI:10.1051/fopen/2020013
J. E. García, V. González-López, G. Tasca
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引用次数: 5

摘要

在本文中,我们在划分马尔可夫模型(PMM)的理论框架内研究了一个特定的结构[参见García Jesús和González-López, Entropy 19,160(2017)]。感兴趣的结构在于底层划分的公式,它定义了过程,其中,除了与过程相关的有限内存0之外,还引入了参数G,允许对过去的额外依赖,以补充通常内存0给出的依赖。我们通过模拟显示,为PMM的经典版本设计的算法如何难以恢复这里研究的结构。这种特定的结构对于模拟来自新解码的人类冠状病毒Covid-19的完整基因组序列是有效的[见Wu等人,Nature 579, 265-269(2020)]。序列轮廓由13个单元(状态空间分区的一部分)表示,对于13个单元中的每一个,它们各自的转移概率被计算为遗传字母表的任何元素。此外,本文提出的结构使我们能够与过去25年收集的其他冠状病毒基因组序列进行比较研究,通过这些研究,我们得出结论,舟山蝙蝠标本中的Covid-19与sars样冠状病毒(sl - cov)相邻[参见Hu等人,emermicrob infections 7,1 - 10(2018)]。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Partition Markov Model for Covid-19 Virus
In this paper, we investigate a specific structure within the theoretical framework of Partition Markov Models (PMM) [see García Jesús and González-López, Entropy 19, 160 (2017)]. The structure of interest lies in the formulation of the underlying partition, which defines the process, in which, in addition to a finite memory o associated with the process, a parameter G is introduced, allowing an extra dependence on the past complementing the dependence given by the usual memory o. We show, by simulations, how algorithms designed for the classic version of the PMM can have difficulties in recovering the structure investigated here. This specific structure is efficient for modeling a complete genome sequence, coming from the newly decoded Coronavirus Covid-19 in humans [see Wu et al., Nature 579, 265–269 (2020)]. The sequence profile is represented by 13 units (parts of the state space’s partition), for each of the 13 units, their respective transition probabilities are computed for any element of the genetic alphabet. Also, the structure proposed here allows us to develop a comparison study with other genomic sequences of Coronavirus, collected in the last 25 years, through which we conclude that Covid-19 is shown next to SARS-like Coronaviruses (SL-CoVs) from bats specimens in Zhoushan [see Hu et al., Emerg Microb Infect 7, 1–10 (2018)].
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