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寄生虫与宿主防御层级之间的剂量依赖性相互作用预示着“虫洞”,即在中等接种量时会延长感染时间。

Dose-dependent interaction of parasites with tiers of host defense predicts "wormholes" that prolong infection at intermediate inoculum sizes.

作者信息

Graham Andrea L, Regoes Roland R

机构信息

Department of Ecology & Evolutionary Biology, Princeton University, Princeton, New Jersey, United States of America.

Institute of Integrative Biology, ETH Zürich, Zurich, Switzerland.

出版信息

PLoS Comput Biol. 2024 Dec 6;20(12):e1012652. doi: 10.1371/journal.pcbi.1012652. eCollection 2024 Dec.

Abstract

Immune responses are induced by parasite exposure and can in turn reduce parasite burden. Despite such apparently simple rules of engagement, key drivers of within-host dynamics, including dose-dependence of defense and infection duration, have proven difficult to predict. Here, we model how varied inoculating doses interact with multi-tiered host defenses at a site of inoculation, by confronting barrier, innate, and adaptive tiers with replicating and non-replicating parasites across multiple orders of magnitude of dose. We find that, in general, intermediate parasite doses generate infections of longest duration because they are sufficient in number to breach barrier defenses, but insufficient to strongly induce subsequent tiers of defense. These doses reveal "wormholes" in defense from which parasites might profit: Deviation from the hypothesis of independent action, which postulates that each parasite has an independent probability of establishing infection, may therefore be widespread. Interestingly, our model predicts local maxima of duration at two doses-one for each tier transition. While some empirical evidence is consistent with nonlinear dose-dependencies, testing the predicted dynamics will require finer-scale dose variation than experiments usually incorporate. Our results help explain varied infection establishment and duration among differentially-exposed hosts and elucidate evolutionary pressures that shape both virulence and defense.

摘要

寄生虫暴露可诱导免疫反应,而免疫反应反过来又能减轻寄生虫负担。尽管这种相互作用的规则看似简单,但包括防御的剂量依赖性和感染持续时间在内的宿主体内动态变化的关键驱动因素却难以预测。在此,我们通过在多个剂量数量级上,使屏障、先天和适应性防御层级与复制型和非复制型寄生虫相互对抗,来模拟不同接种剂量如何在接种部位与多层宿主防御相互作用。我们发现,一般来说,中等寄生虫剂量会导致最长持续时间的感染,因为其数量足以突破屏障防御,但又不足以强烈诱导后续防御层级。这些剂量揭示了防御中的“虫洞”,寄生虫可能从中获益:因此,偏离独立作用假说(该假说假定每个寄生虫都有独立的建立感染的概率)的情况可能很普遍。有趣的是,我们的模型预测在两个剂量处持续时间会出现局部最大值——每个防御层级转变各有一个。虽然一些实证证据与非线性剂量依赖性一致,但要测试预测的动态变化,所需的剂量变化尺度要比通常实验中的更精细。我们的结果有助于解释不同暴露程度宿主之间感染建立和持续时间的差异,并阐明塑造毒力和防御的进化压力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01e7/11654943/e5efcaf7f5f5/pcbi.1012652.g001.jpg

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