一套选择性压力支持果蝇免疫肽等位基因的维持。

Sarah R Mullinax, Andrea M Darby, Anjali Gupta, Patrick Chan, Brittny R Smith, Robert L Unckless
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摘要

先天免疫系统为宿主抵御病原体提供了至关重要的第一道防线。虽然免疫基因通常是基因组中进化最快的基因之一,但在果蝇中,抗菌肽(AMP)是明显的例外。相反,AMPs可能处于平衡选择之下,因此在进化的时间尺度上,群体中保持了多个等位基因。在这项研究中,我们重点研究了果蝇抗菌肽Diptericin A,它具有分离氨基酸多态性,与感染革兰氏阴性菌Providencia rettgeri后的差异生存率有关。Diptericin A也有助于控制常见果蝇肠道微生物,特别是植物乳杆菌的机会性肠道感染。除了对肠道免疫的基因型影响外,我们还发现了强烈的性别特异性影响,在没有功能性双蝶呤A的苍蝇中最为突出。为了进一步表征不同双蝶呤基因型之间微生物组的差异,我们使用16S宏基因组学来研究微生物组的组成。我们使用实验室饲养的苍蝇和野生捕获的苍蝇进行测序,并观察了单个细菌家族的总体组成和差异丰度。总的来说,我们发现,双蝶呤A纯合丝氨酸的苍蝇能够更好地抵御来自雷氏疟原虫的系统性感染,但一般来说,纯合精氨酸苍蝇在喂食普通肠道共生体后寿命更长。我们的研究结果表明,通过性别、系统免疫和肠道微生物组的维持的复杂相互作用,维持蝶呤a基因变异的可能机制。
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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A suite of selective pressures supports the maintenance of alleles of a Drosophila immune peptide.

The innate immune system provides hosts with a crucial first line of defense against pathogens. While immune genes are often among the fastest evolving genes in the genome, in Drosophila , antimicrobial peptides (AMPs) are notable exceptions. Instead, AMPs may be under balancing selection, such that over evolutionary timescales multiple alleles are maintained in populations. In this study, we focus on the Drosophila antimicrobial peptide Diptericin A, which has a segregating amino acid polymorphism associated with differential survival after infection with the Gram-negative bacteria Providencia rettgeri . Diptericin A also helps control opportunistic gut infections by common Drosophila gut microbes, especially those of Lactobacillus plantarum . In addition to genotypic effects on gut immunity, we also see strong sex-specific effects that are most prominent in flies without functional diptericin A . To further characterize differences in microbiomes between different diptericin genotypes, we used 16S metagenomics to look at the microbiome composition. We used both lab reared and wild caught flies for our sequencing and looked at overall composition as well as the differential abundance of individual bacterial families. Overall, we find flies that are homozygous for one allele of diptericin A are better equipped to survive a systemic infection from P. rettgeri , but in general have a shorter lifespans after being fed common gut commensals. Our results suggest a possible mechanism for the maintenance of genetic variation of diptericin A through the complex interactions of sex, systemic immunity, and the maintenance of the gut microbiome.

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