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Amino acid metabolic signaling influences Aedes aegypti midgut microbiome variability

机译:氨基酸代谢信号影响埃及伊蚊中肠微生物组变异性

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摘要

The mosquito midgut microbiota has been shown to influence vector competence for multiple human pathogens. The microbiota is highly variable in the field, and the sources of this variability are not well understood, which limits our ability to understand or predict its effects on pathogen transmission. In this work, we report significant variation in female adult midgut bacterial load between strains of A. aegypti which vary in their susceptibility to dengue virus. Composition of the midgut microbiome was similar overall between the strains, with 81–92% of reads coming from the same five bacterial families, though we did detect differences in the presence of some bacterial families including Flavobacteriaceae and Entobacteriaceae. We conducted transcriptomic analysis on the two mosquito strains that showed the greatest difference in bacterial load, and found that they differ in transcript abundance of many genes implicated in amino acid metabolism, in particular the branched chain amino acid degradation pathway. We then silenced this pathway by targeting multiple genes using RNA interference, which resulted in strain-specific bacterial proliferation, thereby eliminating the difference in midgut bacterial load between the strains. This suggests that the branched chain amino acid (BCAA) degradation pathway controls midgut bacterial load, though the mechanism underlying this remains unclear. Overall, our results indicate that amino acid metabolism can act to influence the midgut microbiota. Moreover, they suggest that genetic or physiological variation in BCAA degradation pathway activity may in part explain midgut microbiota variation in the field.
机译:蚊中肠微生物群已显示影响多种人类病原体的媒介能力。微生物群在该领域中是高度可变的,并且这种可变性的来源尚未得到很好的理解,这限制了我们了解或预测其对病原体传播的影响的能力。在这项工作中,我们报告了埃及埃及曲霉菌株之间的成年中肠细菌载量有显着变化,它们对登革热病毒的敏感性也有所不同。菌株之间中肠微生物组的总体组成相似,其中81–92%的读数来自相同的五个细菌家族,尽管我们确实检测到某些细菌家族(包括黄杆菌科和肠杆菌科)存在差异。我们对显示出最大细菌负载差异的两个蚊子进行了转录组学分析,发现它们在涉及氨基酸代谢的许多基因(尤其是支链氨基酸降解途径)的转录丰度上存在差异。然后,我们通过使用RNA干扰靶向多个基因来沉默该途径,从而导致菌株特异性细菌增殖,从而消除了菌株之间中肠细菌负荷的差异。这表明支链氨基酸(BCAA)降解途径控制中肠细菌负荷,尽管其机制尚不清楚。总的来说,我们的结果表明氨基酸代谢可以影响中肠微生物群。此外,他们认为BCAA降解途径活性的遗传或生理变异可能部分解释了田间中肠微生物群的变异。

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