Sequencing, Fast and Slow: Profiling Microbiomes in Human Samples with Nanopore Sequencing

Yunseol Park; Jeesu Lee; Hyunjin Shim

doi:10.3390/applbiosci2030028

Applied Biosciences (Aug 2023)

Sequencing, Fast and Slow: Profiling Microbiomes in Human Samples with Nanopore Sequencing

Yunseol Park,
Jeesu Lee,
Hyunjin Shim

Affiliations

Yunseol Park: Center for Biosystems and Biotech Data Science, Ghent University Global Campus, Incheon 21985, Republic of Korea
Jeesu Lee: Center for Biosystems and Biotech Data Science, Ghent University Global Campus, Incheon 21985, Republic of Korea
Hyunjin Shim: Center for Biosystems and Biotech Data Science, Ghent University Global Campus, Incheon 21985, Republic of Korea

DOI: https://doi.org/10.3390/applbiosci2030028
Journal volume & issue: Vol. 2, no. 3
pp. 437 – 458

Abstract

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Rapid and accurate pathogen identification is crucial in effectively combating infectious diseases. However, the current diagnostic tools for bacterial infections predominantly rely on century-old culture-based methods. Furthermore, recent research highlights the significance of host–microbe interactions within the host microbiota in influencing the outcome of infection episodes. As our understanding of science and medicine advances, there is a pressing need for innovative diagnostic methods that can identify pathogens and also rapidly and accurately profile the microbiome landscape in human samples. In clinical settings, such diagnostic tools will become a powerful predictive instrument in directing the diagnosis and prognosis of infectious diseases by providing comprehensive insights into the patient’s microbiota. Here, we explore the potential of long-read sequencing in profiling the microbiome landscape from various human samples in terms of speed and accuracy. Using nanopore sequencers, we generate native DNA sequences from saliva and stool samples rapidly, from which each long-read is basecalled in real-time to provide downstream analyses such as taxonomic classification and antimicrobial resistance through the built-in software (<12 h). Subsequently, we utilize the nanopore sequence data for in-depth analysis of each microbial species in terms of host–microbe interaction types and deep learning-based classification of unidentified reads. We find that the nanopore sequence data encompass complex information regarding the microbiome composition of the host and its microbial communities, and also shed light on the unexplored human mobilome including bacteriophages. In this study, we use two different systems of long-read sequencing to give insights into human microbiome samples in the ‘slow’ and ‘fast’ modes, which raises additional inquiries regarding the precision of this novel technology and the feasibility of extracting native DNA sequences from other human microbiomes.

Published in Applied Biosciences

ISSN: 2813-0464 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Chemistry: Organic chemistry: Biochemistry; Science: Biology (General); Technology: Chemical technology: Biotechnology
Website: https://www.mdpi.com/journal/applbiosci

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