How robust are estimates of key parameters in standard viral dynamic models?

IF 4.3 2区生物学 PLoS Computational Biology Pub Date : 2024-04-16 DOI:10.1371/journal.pcbi.1011437

Carolin Zitzmann, Ruian Ke, R. Ribeiro, A. Perelson

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Abstract

Mathematical models of viral infection have been developed, fitted to data, and provide insight into disease pathogenesis for multiple agents that cause chronic infection, including HIV, hepatitis C, and B virus. However, for agents that cause acute infections or during the acute stage of agents that cause chronic infections, viral load data are often collected after symptoms develop, usually around or after the peak viral load. Consequently, we frequently lack data in the initial phase of viral growth, i.e., when pre-symptomatic transmission events occur. Missing data may make estimating the time of infection, the infectious period, and parameters in viral dynamic models, such as the cell infection rate, difficult. However, having extra information, such as the average time to peak viral load, may improve the robustness of the estimation. Here, we evaluated the robustness of estimates of key model parameters when viral load data prior to the viral load peak is missing, when we know the values of some parameters and/or the time from infection to peak viral load. Although estimates of the time of infection are sensitive to the quality and amount of available data, particularly pre-peak, other parameters important in understanding disease pathogenesis, such as the loss rate of infected cells, are less sensitive. Viral infectivity and the viral production rate are key parameters affecting the robustness of data fits. Fixing their values to literature values can help estimate the remaining model parameters when pre-peak data is missing or limited. We find a lack of data in the pre-peak growth phase underestimates the time to peak viral load by several days, leading to a shorter predicted growth phase. On the other hand, knowing the time of infection (e.g., from epidemiological data) and fixing it results in good estimates of dynamical parameters even in the absence of early data. While we provide ways to approximate model parameters in the absence of early viral load data, our results also suggest that these data, when available, are needed to estimate model parameters more precisely.

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标准病毒动态模型中关键参数的估计值有多可靠？

对于包括艾滋病病毒、丙型肝炎病毒和乙型肝炎病毒在内的多种导致慢性感染的病原体，人们已经建立了病毒感染的数学模型，并将其与数据进行了拟合，从而对疾病的发病机理有了深入的了解。然而，对于引起急性感染的病原体或在引起慢性感染的病原体的急性期，病毒载量数据通常是在出现症状后收集的，通常是在病毒载量峰值前后。因此，我们经常缺乏病毒生长初期的数据，即无症状前传播事件发生时的数据。缺失的数据可能会给估算感染时间、感染期和病毒动态模型参数（如细胞感染率）带来困难。然而，如果有额外的信息，如病毒载量达到峰值的平均时间，则可以提高估算的稳健性。在此，我们评估了当病毒载量峰值之前的病毒载量数据缺失时，当我们知道某些参数的值和/或从感染到病毒载量峰值的时间时，关键模型参数估计的稳健性。虽然对感染时间的估计对可用数据的质量和数量很敏感，尤其是高峰前的数据，但对了解疾病发病机制很重要的其他参数（如感染细胞的丢失率）则不太敏感。病毒传染性和病毒产生率是影响数据拟合稳健性的关键参数。将它们的值固定为文献值有助于在峰前数据缺失或有限的情况下估计其余模型参数。我们发现，如果缺乏高峰前生长阶段的数据，病毒载量达到峰值的时间就会被低估数天，从而导致预测的生长阶段缩短。另一方面，即使在缺乏早期数据的情况下，知道感染时间（例如从流行病学数据中）并将其固定下来，也能获得良好的动态参数估计。虽然我们提供了在没有早期病毒载量数据的情况下近似估计模型参数的方法，但我们的结果也表明，如果有这些数据，就需要更精确地估计模型参数。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

PLoS Computational Biology 生物-生化研究方法

CiteScore

7.10

自引率

4.70%

发文量

820

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