key: cord-0923617-pcunojbn authors: Mercier, Alizé; Wilkinson, David A.; Lebarbenchon, Camille; Mavingui, Patrick; Yemadje-Menudier, Luce title: Spread of SARS-CoV-2 Variants on Réunion Island, France, 2021 date: 2022-04-03 journal: Emerg Infect Dis DOI: 10.3201/eid2804.212243 sha: 9112185c2ee0d6a0ec84ac0c9e8cf6f4b8f4b718 doc_id: 923617 cord_uid: pcunojbn In January 2021, after detection of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants, genomic surveillance was established on Réunion Island to track the introduction and spread of SARS-CoV-2 lineages and variants of concern. This system identified 22 SARS-CoV-2 lineages, 71% of which were attributed to the Beta variant In January 2021, after detection of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants, genomic surveillance was established on Réunion Island to track the introduction and spread of SARS-CoV-2 lineages and variants of concern. This system identified 22 SARS-CoV-2 lineages, 71% of which were attributed to the Beta variant RESEARCH LETTERS C oronavirus disease (COVID-19) is a respiratory illness caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). On Réunion Island, an overseas department of France located in the Indian Ocean, the first cases of COVID-19 were detected on March 11, 2020, in a group of travelers (D.A. Wilkinson et al., unpub. data, https://doi.org/10.11 01/2021.01.21.21249623). In response, a regional epidemiologic surveillance focusing on contact tracing and early detection of clusters was conducted. After several months of imported cases and sporadic autochtonous cases, a sharp increase in locally acquired infections was recorded in August 2020, after the return of many Réunion Island residents from travel abroad, primarily mainland France, where the incidence rate was high. The virus subsequently spread throughout the island. In January 2021, after SARS-CoV-2 variants were detected, genomic surveillance was established to track the introduction and spread of SARS-CoV-2 lineages on the island. During January-June 2021, we generated a total of 1,528 genome sequences with >90% coverage using the ARTIC protocol (https:// artic.network/ncov-2019/ncov2019-bioinformaticssop.html) and nanopore technology (MinION; Oxford Nanopore Technologies, https://nanoporetech. com). This collection represents 8.3% of all COV-ID-19 cases on Réunion Island during that period (n = 18,409). Sample selection was pseudo-random; a small proportion of cases was prioritized for sequencing because of atypical epidemiologic or clinical characteristics. Pangolin lineages were assigned to all genomes using Pangolin version 1.2.88 (https://github. com/cov-lineages/pango-designation/releases/ tag/v1.2.88). We present the main findings of genomic surveillance from weeks 1-22, 2021 (January 4-June 6, 2021). We focused on the evolution of the weekly proportions of the 8 most frequent SARS-CoV-2 variants and examined the correlation between the weekly number of confirmed cases and the proportion of sequences identified as Beta variant (B.1.351). We extracted lineage distributions in other islands of the Indian Ocean and South Africa from the GISAID database (http://www. gisaid.org) to investigate the origins of the Beta variant sublineages. We identified 22 SARS-CoV-2 lineages, 71% of which were attributed to the Beta variant (sublineages B.1.351 and B.1.351.2) (Table) . On the basis of available data in the GISAID database, lineage B.1.622 seems to be specific to Réunion Island; no other sequence had been reported elsewhere. Since mid-February 2021 (week 7 of 2021), the Beta variant has become dominant on Réunion Island, despite low-level circulation of the Alpha variant, another variant of concern that was dominant in mainland France and other countries in Europe at that time. We detected a correlation (Spearman ρ = 8.4 × 10 −4 ; p<0.001) between the number of CO-VID-19 cases in January-February 2021 and the number of sequences attributed to the Beta variant, which has been shown to have increased transmissibility (C.A. Pearson et al., unpub. data, https:// cmmid.github.io/topics/covid19/sa-novel-variant. html). Several additional factors could explain the dominance of Beta variant; genetic and epidemiologic factors may have contributed to a founder effect, a higher frequency of virus introductions resulting from holiday travels, possible superspreading events, and local and regional contexts (2) . Indeed, geographic proximity and population movements with Mayotte, another overseas department of France, and Comoros link Réunion Island to South Africa, where Beta variant was first reported (3). This finding, coupled with information from GISAID, suggests that lineage B.1.351.2 was imported to Comoros and Mayotte from South Africa and could have been introduced to Réunion Island from Mayotte (4) (Appendix 1, https://wwwnc.cdc.gov/EID/ article/28/4/21-2243-App1.pdf). This possible introduction from Mayotte is supported by the flow of travelers between the 2 departments and the notable peak in COVID-19 cases that occurred in Mayotte during weeks 1-11, mainly caused by the Beta variant (5). However, analysis of the origin of lineages is strongly affected by each location's capacity to sequence and report genomes in GISAID, which renders comparison between different locations difficult (4). Our study provides valuable insights into the interactions between SARS-CoV-2 lineages on Réunion Island, which represents a closed system with controlled entries, especially when travel restrictions are in place. Additional research on genomic epidemiology and the effect of air travel can further improve understanding of why some variants become dominant over others, particularly in insular contexts. The future of genomic surveillance on Réunion Island will focus on mutation screening to increase reactivity, combined with real-time sequencing, as a robust approach to track the spread of emerging SARS-CoV-2 variants of concern and to inform public health actions (6,7). T he severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) B.1.1.529 (Omicron) variant of concern has been suggested to be more transmissible than previous variants of concern (1). We describe an outbreak caused by the Omicron variant that originated from 1 person with an imported case and rapidly spread within 3 weeks to the community in South Korea. Details of the surveillance and quarantine system in South Korea have been described (2) . Public health officers interviewed case-patients, and to identify links between clusters, we created epidemic curves In South Korea, a November 2021 outbreak caused by severe acute respiratory syndrome coronavirus 2 Omicron variant originated from 1 person with an imported case and spread to households, kindergartens, workplaces, restaurants, and hospitals, resulting in 11 clusters within 3 weeks. An epidemiologic curve indicated rapid community transmission of the Omicron variant. 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B.1.351.2 lineage report COVID-19: weekly report from Mayotte as of 1 Rapid implementation of SARS-CoV-2 sequencing to investigate cases of health-care associated COVID-19: a prospective genomic surveillance study Mutation-specific SARS-CoV-2 PCR screen: rapid and accurate detection of variants of concern and the identification of a newly emerging variant with spike L452R mutation Address for correspondence: Luce Yemadje-Menudier email: luce.menudier@santepubliquefrance.fr Community Transmission of SARS-CoV-2 Omicron Variant Honam Regional Center for Disease Control and Prevention Center for Infectious Disease Control and Prevention We thank all the partners involved in the surveillance of COVID-19 in the Regional Health Agency and the Regional Health Insurance Fund. We acknowledge the key role of the network of sampling laboratories on Réunion Island (CHU, CHOR, Laboratoire de Saint-Benoit, Bioaustral, Réunilab, Cerballiance). We also acknowledge and thank the members of the EMERGEN consortium, as well as Laetitia Ali Oicheih, Elsa Balleydier, Adeline Feri, Javier Castro Alvarez, Sibylle Bernard-Stoecklin, Anna Maisa, Justine Schaeffer, Bruno Coignard, Guillaume Spaccaferri, Bruno Lina, Marie-Alice Simbi, Magali Turpin, Christian Mériau, and Maya Cesari. We are also grateful to the originating and submitting laboratories of the sequences from GISAID database (Appendix 2, https://wwwnc.cdc. gov/EID/article/28/4/21-2243-App1.xlsx). All data submitters may be contacted via the GISAID website (https:// www.gisaid.org). Dr. Mercier is an epidemiologist at Santé publique France, based in the regional office of Réunion. She has a PhD in epidemiology specialized in epidemic intelligence. Her research interests include infectious disease epidemiology, epidemic intelligence, and modeling.