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基于 DNA 的定量和传播阶段计数提供了不同但互补的寄生虫负荷估计:来自啮齿动物球虫(艾美尔球虫)的一个例子。

DNA-based quantification and counting of transmission stages provides different but complementary parasite load estimates: an example from rodent coccidia (Eimeria).

机构信息

Institute for Biology, Department of Molecular Parasitology, Humboldt University Berlin (HU), Philippstr. 13, Haus 14, 10115, Berlin, Germany.

Leibniz-Institut Für Zoo- Und Wildtierforschung (IZW), im Forschungsverbund Berlin e.V., Alfred-Kowalke-Straße 17, 10315, Berlin, Germany.

出版信息

Parasit Vectors. 2022 Feb 4;15(1):45. doi: 10.1186/s13071-021-05119-0.

Abstract

BACKGROUND

Counting parasite transmission stages in faeces is the classical measurement to quantify "parasite load". DNA-based quantifications of parasite intensities from faecal samples are relatively novel and often validated against such counts. When microscopic and molecular quantifications do not correlate, it is unclear whether oocyst counts or DNA-based intensity better reflects biologically meaningful concepts. Here, we investigate this issue using the example of Eimeria ferrisi (Coccidia), an intracellular parasite of house mice (Mus musculus).

METHODS

We performed an infection experiment of house mice with E. ferrisi, in which the intensity of infection correlates with increased health impact on the host, measured as temporary weight loss during infection. We recorded the number of parasite transmissive stages (oocysts) per gram of faeces (OPG) and, as a DNA-based measurement, the number of Eimeria genome copies per gram of faeces for 10 days post-infection (dpi). We assessed weight loss relative to the day of experimental infection as a proxy of host health and evaluated whether DNA or oocyst counts are better predictors of host health.

RESULTS

Absolute quantification of Eimeria DNA and oocyst counts showed similar but slightly diverging temporal patterns during 10 dpi. We detected Eimeria DNA earlier than the first appearance of oocysts in faeces. Additionally, Eimeria OPGs within each dpi did not explain parasite DNA intensity. Early dpi were characterized by high DNA intensity with low oocyst counts, while late infections showed the opposite pattern. The intensity of Eimeria DNA was consistently a stronger predictor of either maximal weight loss (1 value per animal during the infection course) or weight loss on each day during the experiment when controlling for between-dpi and between-individual variance.

CONCLUSIONS

Eimeria ferrisi oocyst counts correlate weakly with parasite intensity assessed through DNA quantification. DNA is likely partially derived from life-cycle stages other than transmissive oocysts. DNA-based intensities predict health outcomes of infection for the host more robustly than counts of transmissive stages. We conclude that DNA-based quantifications should not necessarily require validation against counts of transmissive stages. Instead, DNA-based load estimates should be evaluated as complementary sources of information with potential specific biological relevance for each host-parasite system.

摘要

背景

在粪便中计数寄生虫传播阶段是量化“寄生虫负荷”的经典方法。基于 DNA 的粪便样本寄生虫强度定量分析相对较新,通常与此类计数进行验证。当显微镜检查和分子定量分析不相关时,尚不清楚卵囊计数或基于 DNA 的强度更能反映有意义的生物学概念。在这里,我们使用肠内原虫(球虫)的例子来研究这个问题,肠内原虫是家鼠(Mus musculus)的一种细胞内寄生虫。

方法

我们对家鼠进行了肠内原虫感染实验,其中感染强度与宿主健康的影响程度相关,用感染期间暂时的体重减轻来衡量。我们记录了每克粪便中的寄生虫传播阶段(卵囊)数量(OPG)和感染后 10 天每克粪便中的肠内原虫基因组拷贝数(Eimeria 基因组拷贝数)。我们将相对于实验感染日的体重减轻作为宿主健康的替代指标,并评估 DNA 或卵囊计数哪个更好地预测宿主健康。

结果

在 10 天的时间里,肠内原虫 DNA 的绝对定量和卵囊计数表现出相似但略有不同的时间模式。我们检测到肠内原虫 DNA 的时间早于粪便中首次出现卵囊的时间。此外,每个 dpi 内的肠内原虫 OPG 并不能解释寄生虫 DNA 强度。早期 dpi 表现为高 DNA 强度和低卵囊计数,而晚期感染则表现出相反的模式。肠内原虫 DNA 强度始终是预测感染过程中最大体重减轻(每个动物在感染过程中的 1 个值)或实验期间每天体重减轻的更有力指标,当控制 dpi 之间和个体之间的变异性时。

结论

肠内原虫卵囊计数与通过 DNA 定量评估的寄生虫强度相关性较弱。DNA 可能部分来自于非传播性卵囊的生命周期阶段。基于 DNA 的强度比传播性阶段的计数更能预测宿主感染的健康结果。我们得出结论,基于 DNA 的定量分析不一定需要针对传播性阶段的计数进行验证。相反,应将基于 DNA 的负荷估计值作为补充信息源进行评估,每个宿主-寄生虫系统都具有潜在的特定生物学相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b1e/8815199/19ba4684fb01/13071_2021_5119_Fig1_HTML.jpg

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