SARS-CoV-2 variants in Paraguay : detection and surveillance with an economical and scalable molecular protocol
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Martínez Pereira, Iara Magaly; Nguyen, Phuong-Vi; Su, Maxwell; Cardozo Segovia, Fátima María; Valenzuela, Adriana Beatriz; Franco, Laura Ximena; Galeano, María Eugenia; Rojas, Leticia Elizabeth; Díaz Acosta, Chyntia Carolina; Fernández, Jonás; Ortíz, Joel; del Puerto Rodas, Ramona Florencia; Mendoza Torres, Laura Patricia; Nara, Eva; Rojas Segovia, Alejandra María; Waggoner, Jesse J.Date of publishing
2022-04-22Type of publication
info:eu-repo/semantics/articleSubject(s)
COVID-19/diagnóstico
COVID-19/epidemiología
Humanos
Paraguay/epidemiología
SARS-CoV-2/genética
COVID-19/diagnosis
COVID-19/epidemiology
Humans
Paraguay/epidemiology
SARS-CoV-2/genetics
Paraguay
Real-time RT-PCR
SARS-CoV-2
Variants
COVID-19/epidemiología
Humanos
Paraguay/epidemiología
SARS-CoV-2/genética
COVID-19/diagnosis
COVID-19/epidemiology
Humans
Paraguay/epidemiology
SARS-CoV-2/genetics
Paraguay
Real-time RT-PCR
SARS-CoV-2
Variants
Abstract
SARS-CoV-2 variant detection relies on resource-intensive whole-genome sequencing methods. We sought to develop a scalable protocol for variant detection and surveillance in Paraguay, pairing rRT-PCR for spike mutations with Nanopore sequencing. A total of 201 acute-phase nasopharyngeal samples were included. Samples were positive for the SARS-CoV-2 N2 target and tested with the Spike SNP assay to detect mutations associated with the following variants: alpha (501Y), beta/gamma (417variant/484K/501Y), delta (452R/478K), and lambda (452Q/490S). Spike SNP calls were confirmed using amplicon (Sanger) sequencing and whole-genome (Nanopore) sequencing on a subset of samples with confirmed variant lineages. Samples had a mean N2 Ct of 20.8 (SD 5.6); 198/201 samples (98.5%) tested positive in the Spike SNP assay. The most common genotype was 417variant/484K/501Y, detected in 102/198 samples (51.5%), which was consistent with the P.1 lineage (gamma variant) in Paraguay. No mutations (K417 only) were found in 64/198 (32.3%), and K417/484K was identified in 22/198 (11.1%), consistent with P.2 (zeta). Seven samples (3.5%) tested positive for 452R without 478K, and one sample with genotype K417/501Y was confirmed as B.1.1.7 (alpha). The results were confirmed using Sanger sequencing in 181/181 samples, and variant calls were consistent with Nanopore sequencing in 29/29 samples. The Spike SNP assay could improve population-level surveillance for mutations associated with SARS-CoV-2 variants and inform the judicious use of sequencing resources.