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对早产儿早期定植和医院病房中真核生物种群进行基于基因组解析的宏基因组学研究。

Genome-resolved metagenomics of eukaryotic populations during early colonization of premature infants and in hospital rooms.

机构信息

Department of Plant and Microbial Biology, University of California, Berkeley, CA, USA.

Present address: Kaleido Biosciences, Bedford, MA, USA.

出版信息

Microbiome. 2019 Feb 15;7(1):26. doi: 10.1186/s40168-019-0638-1.

Abstract

BACKGROUND

Fungal infections are a significant cause of mortality and morbidity in hospitalized preterm infants, yet little is known about eukaryotic colonization of infants and of the neonatal intensive care unit as a possible source of colonizing strains. This is partly because microbiome studies often utilize bacterial 16S rRNA marker gene sequencing, a technique that is blind to eukaryotic organisms. Knowledge gaps exist regarding the phylogeny and microdiversity of eukaryotes that colonize hospitalized infants, as well as potential reservoirs of eukaryotes in the hospital room built environment.

RESULTS

Genome-resolved analysis of 1174 time-series fecal metagenomes from 161 premature infants revealed fungal colonization of 10 infants. Relative abundance levels reached as high as 97% and were significantly higher in the first weeks of life (p = 0.004). When fungal colonization occurred, multiple species were present more often than expected by random chance (p = 0.008). Twenty-four metagenomic samples were analyzed from hospital rooms of six different infants. Compared to floor and surface samples, hospital sinks hosted diverse and highly variable communities containing genomically novel species, including from Diptera (fly) and Rhabditida (worm) for which genomes were assembled. With the exception of Diptera and two other organisms, zygosity of the newly assembled diploid eukaryote genomes was low. Interestingly, Malassezia and Candida species were present in both room and infant gut samples.

CONCLUSIONS

Increased levels of fungal co-colonization may reflect synergistic interactions or differences in infant susceptibility to fungal colonization. Discovery of eukaryotic organisms that have not been sequenced previously highlights the benefit of genome-resolved analyses, and low zygosity of assembled genomes could reflect inbreeding or strong selection imposed by room conditions.

摘要

背景

真菌感染是住院早产儿死亡和发病的重要原因,但人们对婴儿和新生儿重症监护病房(NICU)中真核生物的定植情况以及这些环境是否可能成为定植菌株的来源知之甚少。这在一定程度上是因为微生物组研究通常利用细菌 16S rRNA 标记基因测序,而该技术无法检测真核生物。在定植于住院婴儿的真核生物的系统发育和微观多样性,以及医院室内环境中真核生物的潜在储库方面,存在知识空白。

结果

对 161 名早产儿的 1174 个时间序列粪便宏基因组进行了基因组解析分析,结果显示有 10 名婴儿发生了真菌感染。相对丰度水平高达 97%,且在生命的最初几周显著升高(p=0.004)。当发生真菌感染时,多个物种的存在频率高于随机出现的频率(p=0.008)。对来自 6 名不同婴儿的 24 个宏基因组样本进行了分析。与地面和表面样本相比,医院水槽中的样本包含更多的多样化和高度可变的群落,其中包括来自双翅目(蝇类)和毛圆目(线虫)的新物种,这些物种的基因组被组装。除了双翅目和另外两个生物体外,新组装的二倍体真核生物基因组的同质性较低。有趣的是,马拉色菌和假丝酵母在房间和婴儿肠道样本中均有存在。

结论

真菌共同定植水平的增加可能反映了协同相互作用或婴儿对真菌感染易感性的差异。发现以前未测序的真核生物突出了基因组解析分析的优势,而组装基因组的同质性较低可能反映了近亲繁殖或房间条件造成的强烈选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9abd/6377789/2886497b6baf/40168_2019_638_Fig1_HTML.jpg

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