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MinION™ Nanopore Sequencing of Skin Microbiome 16S and 16S-23S rRNA Gene Amplicons

Miquel Rozas, François Brillet, Chris Callewaert, Bernhard Paetzold

2022Frontiers in Cellular and Infection Microbiology39 citationsDOIOpen Access PDF

Abstract

Human skin microbiome dysbiosis can have clinical consequences. Characterizing taxonomic composition of bacterial communities associated with skin disorders is important for dermatological advancement in both diagnosis and novel treatments. This study aims to analyze and improve the accuracy of taxonomic classification of skin bacteria with MinION™ nanopore sequencing using a defined skin mock community and a skin microbiome sample. We compared the Oxford Nanopore Technologies recommended procedures and concluded that their protocols highly bias the relative abundance of certain skin microbiome genera, most notably a large overrepresentation of Staphylococcus and underrepresentation of Cutibacterium and Corynebacterium . We demonstrated that changes in the amplification protocols improved the accuracy of the taxonomic classification for these three main skin bacterial genera. This study shows that MinION™ nanopore could be an efficient technology for full-length 16S rRNA sequencing; however, the analytical advantage is strongly influenced by the methodologies. The suggested alternatives in the sample processing improved characterization of a complex skin microbiome community using MinION™ nanopore sequencing.

Topics & Concepts

MinionNanopore sequencingMicrobiomeBiologyMetagenomicsAmpliconComputational biology16S ribosomal RNANanoporeDysbiosisAmplicon sequencingRibosomal RNAHuman microbiomeDNA sequencingGeneticsBacteriaGenePolymerase chain reactionNanotechnologyMaterials scienceBacterial Identification and Susceptibility TestingClostridium difficile and Clostridium perfringens researchInfections and bacterial resistance
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