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冈比亚按蚊肠道上皮对粘质沙雷氏菌反应的遗传剖析

Genetic dissection of Anopheles gambiae gut epithelial responses to Serratia marcescens.

作者信息

Stathopoulos Stavros, Neafsey Daniel E, Lawniczak Mara K N, Muskavitch Marc A T, Christophides George K

机构信息

Department of Life Sciences, Imperial College London, London, United Kingdom.

Broad Institute, Cambridge, Massachusetts, United States of America.

出版信息

PLoS Pathog. 2014 Mar 6;10(3):e1003897. doi: 10.1371/journal.ppat.1003897. eCollection 2014 Mar.

Abstract

Genetic variation in the mosquito Anopheles gambiae profoundly influences its ability to transmit malaria. Mosquito gut bacteria are shown to influence the outcome of infections with Plasmodium parasites and are also thought to exert a strong drive on genetic variation through natural selection; however, a link between antibacterial effects and genetic variation is yet to emerge. Here, we combined SNP genotyping and expression profiling with phenotypic analyses of candidate genes by RNAi-mediated silencing and 454 pyrosequencing to investigate this intricate biological system. We identified 138 An. gambiae genes to be genetically associated with the outcome of Serratia marcescens infection, including the peptidoglycan recognition receptor PGRPLC that triggers activation of the antibacterial IMD/REL2 pathway and the epidermal growth factor receptor EGFR. Silencing of three genes encoding type III fibronectin domain proteins (FN3Ds) increased the Serratia load and altered the gut microbiota composition in favor of Enterobacteriaceae. These data suggest that natural genetic variation in immune-related genes can shape the bacterial population structure of the mosquito gut with high specificity. Importantly, FN3D2 encodes a homolog of the hypervariable pattern recognition receptor Dscam, suggesting that pathogen-specific recognition may involve a broader family of immune factors. Additionally, we showed that silencing the gene encoding the gustatory receptor Gr9 that is also associated with the Serratia infection phenotype drastically increased Serratia levels. The Gr9 antibacterial activity appears to be related to mosquito feeding behavior and to mostly rely on changes of neuropeptide F expression, together suggesting a behavioral immune response following Serratia infection. Our findings reveal that the mosquito response to oral Serratia infection comprises both an epithelial and a behavioral immune component.

摘要

冈比亚按蚊的基因变异深刻影响其传播疟疾的能力。研究表明,蚊子肠道细菌会影响疟原虫感染的结果,并且还被认为通过自然选择对基因变异产生强大驱动作用;然而,抗菌作用与基因变异之间的联系尚未显现。在此,我们将单核苷酸多态性(SNP)基因分型和表达谱分析与通过RNA干扰介导的沉默和454焦磷酸测序对候选基因进行的表型分析相结合,以研究这个复杂的生物系统。我们鉴定出138个与粘质沙雷氏菌感染结果存在遗传关联的冈比亚按蚊基因,包括触发抗菌IMD/REL2途径激活的肽聚糖识别受体PGRPLC和表皮生长因子受体EGFR。对三个编码III型纤连蛋白结构域蛋白(FN3Ds)的基因进行沉默,会增加沙雷氏菌载量,并改变肠道微生物群组成,有利于肠杆菌科细菌生长。这些数据表明,免疫相关基因的自然遗传变异能够高度特异性地塑造蚊子肠道的细菌种群结构。重要的是,FN3D2编码高变模式识别受体Dscam的同源物,这表明病原体特异性识别可能涉及更广泛的免疫因子家族。此外,我们发现,对同样与沙雷氏菌感染表型相关的味觉受体Gr9编码基因进行沉默,会大幅提高沙雷氏菌水平。Gr9的抗菌活性似乎与蚊子的取食行为有关,并且主要依赖于神经肽F表达的变化,这共同表明沙雷氏菌感染后会产生行为免疫反应。我们的研究结果表明,蚊子对口服沙雷氏菌感染的反应包括上皮免疫和行为免疫成分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/282a/3946313/f591a358995c/ppat.1003897.g001.jpg

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