Evaluation of a multiplexed tiling PCR scheme for whole-genome amplification of hepatitis B virus using Oxford Nanopore sequencing

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This paper evaluated a previously published tiling PCR primer scheme (Ringlander et al., 2022) for whole-genome amplification of hepatitis B virus in clinical serum or plasma samples, adapted for Oxford Nanopore sequencing and covering HBV genotypes A–E across a wide Ct range. The authors compared two multiplexing strategies—a single pooled reaction containing all primers versus a two-pool approach with non-overlapping amplicons—and processed reads with a Nanopore analysis pipeline to assess genome coverage and amplicon performance. Median genome coverage was about 50% overall, with recovery varying from complete failure to nearly full genomes; pooling strategy had little consistent effect, while amplification efficiency differed strongly by individual amplicon. The study reports that genome coverage correlated with Ct values and that uneven performance of amplicons 6–10 commonly led to incomplete genome recovery, limiting consistent full-genome results. The paper does not explicitly discuss endometriosis or adenomyosis; it was included in the corpus via a keyword match in the upstream search index.

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Full text loading... Abstract Here we evaluated the performance of a previously published tiling PCR primer scheme by Ringlander et al. (2022) for whole-genome amplification of Hepatitis B virus (HBV) in combination with Oxford Nanopore sequencing. The primer set originally developed for Ion Torrent sequencing was adapted by removing platform-specific adapters and tested using clinical serum or plasma samples submitted for routine HBV genotyping and resistance testing. Two multiplexing strategies were compared: a single PCR pool containing all primers and a two-pool strategy with non-overlapping amplicons. Sequencing reads were processed using a Nanopore analysis pipeline, and genome coverage and amplicon performance were compared across samples spanning a wide Ct range and representing HBV genotypes A–E. Across all samples, the median genome coverage was approximately 50%, although recovery varied widely, ranging from complete failure to nearly full genomes. Combining all primers into a single PCR reaction, or separating overlapping amplicons into different reactions, had little overall impact on genome recovery, and no consistent differences between the two pooling strategies were observed. In contrast, amplification efficiency differed markedly between individual amplicons. Amplicons 1–5 generally produced higher sequencing depth, whereas amplicons 6–10 frequently showed low coverage and contributed to incomplete genome recovery. Genome coverage was strongly associated with Ct values, with higher coverage observed in samples with lower Ct values, while coverage was broadly similar across genotypes. These results demonstrate that the Ringlander et al. primer scheme can be adapted for multiplex PCR and Nanopore sequencing of HBV, but uneven amplicon performance limits consistent full-genome recovery and highlights the need for further optimization of HBV tiling PCR designs. - Received: - Version Posted:

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