Title | Complete Genomic Characterization of Global Pathogens, Respiratory Syncytial Virus (RSV), and Human Norovirus (HuNoV) Using Probe-based Capture Enrichment. |
Publication Type | Journal Article |
Year of Publication | 2024 |
Authors | Bhamidipati, SV, Surathu, A, Chao, H, Agustinho, DP, Xiang, Q, Kottapalli, K, Santhanam, A, Momin, Z, Walker, K, Menon, VK, Weissenberger, G, Emerick, N, Mahjabeen, F, Meng, Q, Hu, J, Sucgang, R, Henke, D, Sedlazeck, FJ, Khan, Z, Metcalf, GA, Avadhanula, V, Piedra, PA, Ramani, S, Atmar, RL, Estes, MK, Petrosino, JF, Gibbs, RA, Muzny, DM, Cregeen, SJavornik, Doddapaneni, H |
Journal | bioRxiv |
Date Published | 2024 Sep 16 |
ISSN | 2692-8205 |
Abstract | Respiratory syncytial virus (RSV) is the leading cause of lower respiratory tract infections in children worldwide, while human noroviruses (HuNoV) are a leading cause of epidemic and sporadic acute gastroenteritis. Generating full-length genome sequences for these viruses is crucial for understanding viral diversity and tracking emerging variants. However, obtaining high-quality sequencing data is often challenging due to viral strain variability, quality, and low titers. Here, we present a set of comprehensive oligonucleotide probe sets designed from 1,570 RSV and 1,376 HuNoV isolate sequences in GenBank. Using these probe sets and a capture enrichment sequencing workflow, 85 RSV positive nasal swab samples and 55 (49 stool and six human intestinal enteroids) HuNoV positive samples encompassing major subtypes and genotypes were characterized. The Ct values of these samples ranged from 17.0-29.9 for RSV, and from 20.2-34.8 for HuNoV, with some HuNoV having below the detection limit. The mean percentage of post-processing reads mapped to viral genomes was 85.1% for RSV and 40.8% for HuNoV post-capture, compared to 0.08% and 1.15% in pre-capture libraries, respectively. Full-length genomes were>99% complete in all RSV positive samples and >96% complete in 47/55 HuNoV positive samples-a significant improvement over genome recovery from pre-capture libraries. RSV transcriptome (subgenomic mRNAs) sequences were also characterized from this data. Probe-based capture enrichment offers a comprehensive approach for RSV and HuNoV genome sequencing and monitoring emerging variants. |
DOI | 10.1101/2024.09.16.613242 |
Alternate Journal | bioRxiv |
PubMed ID | 39345650 |
PubMed Central ID | PMC11429736 |
Grant List | U19 AI144297 / AI / NIAID NIH HHS / United States |