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首页> 外文期刊>Frontiers in Microbiology >Leucine-Rich Immune Factor APL1 Is Associated With Specific Modulation of Enteric Microbiome Taxa in the Asian Malaria Mosquito Anopheles stephensi
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Leucine-Rich Immune Factor APL1 Is Associated With Specific Modulation of Enteric Microbiome Taxa in the Asian Malaria Mosquito Anopheles stephensi

机译:富含亮氨酸的免疫因子APL1与亚洲疟疾蚊子的肠道微生物群分类群的特异性调节相关 anopheles stephensi

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摘要

The commensal gut microbiome is contained by the enteric epithelial barrier, but little is known about the degree of specificity of host immune barrier interactions for particular bacterial taxa. Here, we show that depletion of leucine-rich repeat immune factor APL1 in the Asian malaria mosquito Anopheles stephensi is associated with higher midgut abundance of just the family Enterobacteraceae , and not generalized dysbiosis of the microbiome. The effect is explained by the response of a narrow clade containing two main taxa related to Klebsiella and Cedecea . Analysis of field samples indicate that these two taxa are recurrent members of the wild Anopheles microbiome. Triangulation using sequence and functional data incriminated relatives of C. neteri and Cedecea NFIX57 as candidates for the Cedecea component, and K. michiganensis , K. oxytoca , and K.sp. LTGPAF-6F as candidates for the Klebsiella component. APL1 presence is associated with host ability to specifically constrain the abundance of a narrow microbiome clade of the Enterobacteraceae , and the immune factor may promote homeostasis of this clade in the enteric microbiome for host benefit.
机译:非肠道上皮屏障含有共生肠道微生物组,但对于特定细菌分类群的宿主免疫屏障相互作用的特异性很少。在这里,我们表明亚洲疟疾中富含亮氨酸的重复免疫因子APL1的耗尽与家庭肠杆菌的较高的中小型丰富有关,而不是微生物组的概括性消化不良有关。狭窄的思路的响应解释了含有与Klebsiella和Cedecea相关的两个主要分类群的狭窄思克的响应。场样品的分析表明,这两个征征是野生肌肉微生物组的复发成员。使用序列和功能性数据的三角算法C. neteri和Cedecea Nfix57作为Cedecea组分的候选者,K.Michiganensis,K. Oxytoca和K.Sp. LTGPAF-6F作为Klebsiella组分的候选者。 APL1存在与宿主能力有关,具体限制肠杆菌基因的狭窄微生物组的丰度,并且免疫因子可以促进肠道微生物组中该岩石的稳态,以进行宿主。

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