Department of Biology, Lund University, Lund, Sweden.
Center for Conservation Genomics, Smithsonian Conservation Biology Institute, Washington, DC, USA.
Microbiome. 2020 Oct 12;8(1):147. doi: 10.1186/s40168-020-00925-7.
Imbalances in the gut microbial community (dysbiosis) of vertebrates have been associated with several gastrointestinal and autoimmune diseases. However, it is unclear which taxa are associated with gut dysbiosis, and if particular gut regions or specific time periods during ontogeny are more susceptible. We also know very little of this process in non-model organisms, despite an increasing realization of the general importance of gut microbiota for health.
Here, we examine the changes that occur in the microbiome during dysbiosis in different parts of the gastrointestinal tract in a long-lived bird with high juvenile mortality, the ostrich (Struthio camelus). We evaluated the 16S rRNA gene composition of the ileum, cecum, and colon of 68 individuals that died of suspected enterocolitis during the first 3 months of life (diseased individuals), and of 50 healthy individuals that were euthanized as age-matched controls. We combined these data with longitudinal environmental and fecal sampling to identify potential sources of pathogenic bacteria and to unravel at which stage of development dysbiosis-associated bacteria emerge.
Diseased individuals had drastically lower microbial alpha diversity and differed substantially in their microbial beta diversity from control individuals in all three regions of the gastrointestinal tract. The clear relationship between low diversity and disease was consistent across all ages in the ileum, but decreased with age in the cecum and colon. Several taxa were associated with mortality (Enterobacteriaceae, Peptostreptococcaceae, Porphyromonadaceae, Clostridium), while others were associated with health (Lachnospiraceae, Ruminococcaceae, Erysipelotrichaceae, Turicibacter, Roseburia). Environmental samples showed no evidence of dysbiosis-associated bacteria being present in either the food, water, or soil substrate. Instead, the repeated fecal sampling showed that pathobionts were already present shortly after hatching and proliferated in individuals with low microbial diversity, resulting in high mortality several weeks later.
Identifying the origins of pathobionts in neonates and the factors that subsequently influence the establishment of diverse gut microbiota may be key to understanding dysbiosis and host development. Video Abstract.
脊椎动物肠道微生物群落(失调)的失衡与多种胃肠道和自身免疫性疾病有关。然而,目前尚不清楚哪些分类群与肠道失调有关,以及特定的肠道区域或个体发育过程中的特定时间是否更容易受到影响。尽管人们越来越认识到肠道微生物群对健康的普遍重要性,但我们对非模式生物的这一过程也知之甚少。
在这里,我们研究了在一种具有高幼体死亡率的长寿鸟类(鸵鸟)的胃肠道不同部位发生失调时微生物组的变化。我们评估了 68 名个体的回肠、盲肠和结肠的 16S rRNA 基因组成,这些个体在生命的前 3 个月死于疑似肠炎(患病个体),并评估了 50 名作为年龄匹配对照而安乐死的健康个体。我们将这些数据与纵向环境和粪便采样相结合,以确定潜在的病原菌来源,并揭示失调相关细菌在哪个发育阶段出现。
患病个体的微生物 alpha 多样性明显降低,在回肠、盲肠和结肠三个区域,其微生物 beta 多样性与对照个体有很大差异。低多样性与疾病之间的明确关系在回肠的所有年龄段都保持一致,但在盲肠和结肠中随年龄而降低。一些分类群与死亡率相关(肠杆菌科、消化链球菌科、卟啉单胞菌科、梭菌科),而另一些与健康相关(毛螺菌科、瘤胃球菌科、真杆菌科、Turicibacter、玫瑰杆菌属)。环境样本显示,食物、水或土壤基质中不存在与失调相关的细菌。相反,重复的粪便采样显示,pathobionts 早在孵化后不久就已存在,并在微生物多样性较低的个体中增殖,导致数周后死亡率升高。
确定新生个体中 pathobionts 的起源以及随后影响多样化肠道微生物群建立的因素可能是理解肠道失调和宿主发育的关键。
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