Population-based nanopore sequencing of the HIV-1 pangenome to identify drug resistance mutations

Author:

Ode HirotakaORCID,Matsuda Masakazu,Shigemi Urara,Mori MikikoORCID,Yamamura Yoshimi,Nakata Yoshihiro,Okazaki Reiko,Kubota Mai,Setoyama Yuka,Imahashi MayumiORCID,Yokomaku YoshiyukiORCID,Iwatani YasumasaORCID

Abstract

AbstractHIV-1 drug resistance genotypic tests have primarily been performed by Sanger sequencing of gene segments encoding different drug target proteins. Since the number of targets has increased with the addition of a new class of antiretroviral drugs, a simple high-throughput system for assessing nucleotide sequences throughout the HIV-1 genome is required. Here, we developed a new solution using nanopore sequencing of viral pangenomes amplified by PCR. Benchmark tests using HIV-1 molecular clones demonstrated an accuracy of up to 99.9%. In addition, validation tests of our protocol in 106 clinical samples demonstrated high concordance of drug resistance and tropism genotypes (92.5% and 98.1%, respectively) between the nanopore sequencing-based results and archived clinical determinations made based on Sanger sequencing data. These results suggest that our new approach will be a powerful solution for the comprehensive survey of HIV-1 drug resistance mutations in clinical settings.

Funder

Japan Society for the Promotion of Science

Japan Agency for Medical Research and Development

Publisher

Springer Science and Business Media LLC

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