首页> 外文期刊>Frontiers in Marine Science >Metatranscriptome analysis of the reef-building coral Orbicella faveolata indicates holobiont response to coral disease
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Metatranscriptome analysis of the reef-building coral Orbicella faveolata indicates holobiont response to coral disease

机译:对造礁珊瑚Orbicella faveolata的转录组分析表明,holobiont对珊瑚病有反应

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White Plague Disease (WPD) is implicated in coral reef decline in the Caribbean and is characterized by microbial community shifts in coral mucus and tissue. Studies thus far have focused on assessing microbial communities or the identification of specific pathogens, yet few have addressed holobiont response across metaorganism compartments in coral disease. Here, we report on the first metatranscriptomic assessment of the coral host, algal symbiont, and microbial compartment in order to survey holobiont structure and function in healthy and diseased samples from Orbicella faveolata collected at reef sites off Puerto Rico. Our data indicate metaorganism-wide as well as compartment-specific responses to WPD. Gene expression changes in the diseased coral host involved proteins playing a role in innate immunity, cytoskeletal integrity, cell adhesion, oxidative stress, chemical defense, and retroelements. In contrast, the algal symbiont showed comparatively few expression changes, but of large magnitude, of genes related to stress, photosynthesis, and metal transport. Concordant with the coral host response, the bacterial compartment showed increased abundance of heat shock proteins, genes related to oxidative stress, DNA repair, and potential retroelement activity. Importantly, analysis of the expressed bacterial gene functions establishes the participation of multiple bacterial families in WPD pathogenesis and also suggests a possible involvement of viruses and/or phages in structuring the bacterial assemblage. In this study, we implement an experimental approach to partition the coral holobiont and resolve compartment- and taxa-specific responses in order to understand metaorganism function in coral disease.
机译:白鼠疫病(WPD)与加勒比海珊瑚礁的衰退有关,其特征是珊瑚黏液和组织中的微生物群落发生了变化。迄今为止,研究集中在评估微生物群落或特定病原体的鉴定上,但很少有研究涉及珊瑚病中跨整个微生物区室的全生命周期反应。在这里,我们报道了对珊瑚宿主,藻类共生体和微生物区隔的首次转录组学评估,目的是调查在波多黎各海域的珊瑚礁地点收集的健康和患病样品中的健康和患病样品中的整体结构和功能。我们的数据显示了对WPD的全有机物以及针对隔室的反应。患病珊瑚宿主中的基因表达变化涉及蛋白质,这些蛋白质在先天免疫,细胞骨架完整性,细胞粘附,氧化应激,化学防御和逆转录作用中起作用。相反,藻类共生体显示出与胁迫,光合作用和金属转运相关的基因的表达变化相对较少,但幅度较大。与珊瑚宿主反应一致,细菌区室显示出增加的热休克蛋白,与氧化应激,DNA修复和潜在的逆转录活性有关的基因。重要的是,对表达的细菌基因功能的分析建立了WPD发病机制中多个细菌家族的参与,也暗示了病毒和/或噬菌体可能参与了细菌组装的构建。在这项研究中,我们实施了一种实验方法来划分珊瑚全虹膜并解析特定于舱室和分类单元的反应,以了解珊瑚病中的代谢生物功能。

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