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Volume 27, Number 6—June 2021
Online Report

Proposal for Human Respiratory Syncytial Virus Nomenclature below the Species Level

Vahid Salimi, Mariana Viegas1, Alfonsina Trento1, Charles N. Agoti, Larry J. Anderson, Vasanthi Avadhanula, Justin Bahl, Louis Bont, J. Rodney Brister, Patricia A. Cane, Mónica Galiano, Barney S. Graham, Eneida L. Hatcher, Orienka Hellferscee, David M. Henke, Siddhivinayak Hirve, Sandra Jackson, Els Keyaerts, Leyla Kragten-Tabatabaie, Stephen Lindstrom, Inne Nauwelaers, D. James Nokes, Peter J. Openshaw, Teresa C. Peret, Pedro A. Piedra, Kaat Ramaekers, Annabel Rector, Nídia Sequeira Trovão, Anne von Gottberg, Maria Zambon, Wenqing Zhang, Thomas C. Williams, Ian G. Barr2Comments to Author , and Ursula J. Buchholz2Comments to Author 
Author affiliations: Tehran University of Medical Sciences, Tehran, Iran (V. Salimi); Hospital de Niños Dr. Ricardo Gutiérrez, Buenos Aires, Argentina (M. Viegas); National Center of Biotechnology, Madrid, Spain (A. Trento); KEMRI-Wellcome Trust Research Programme, Kilifi, Kenya (C.N. Agoti, D.J. Nokes); Emory University, Atlanta, Georgia, USA (L.J. Anderson); Baylor College of Medicine, Houston, Texas, USA (V. Avadhanula, D.M. Henke, P.A. Piedra); University of Georgia, Athens, Georgia, USA (J. Bahl); University Medical Center, Utrecht, the Netherlands (L. Bont); National Center for Biotechnology Information, Bethesda, Maryland, USA (J.R. Brister, E.L. Hatcher); Public Health England, London, UK (P.A. Cane, M. Galiano, I. Nauwelaers, M. Zambon); Francis Crick Institute, London (M. Galiano); National Institute of Allergy and Infectious Diseases, Bethesda (B.S. Graham, U.J. Buchholz); National Institute for Communicable Diseases of the National Health Laboratory Service, Johannesburg, South Africa (O. Hellferscee, A. von Gottberg); W; orld Health Organization, Geneva, Switzerland (S. Hirve, S. Jackson, W. Zhang); University Hospitals Leuven, Leuven, Belgium (E. Keyaerts); ReSViNET Foundation, Zeist, the Netherlands (L. Kragten-Tabatabaie); Julius Clinical, Zeist (L. Kragten-Tabatabaie); Centers for Disease Control and Prevention, Atlanta (S. Lindstrom, T. Peret); Imperial College London, London (I. Nauwelaers, P. Openshaw); Rega Institute, Leuven (K. Ramaekers, A. Rector); Fogarty International Center, Bethesda (N. Sequeira Trovão); University of Edinburgh, Edinburgh, Scotland, UK (T.C. Williams); Peter Doherty Institute for Infection & Immunity, Melbourne, Victoria, Australia (I. Barr)

Main Article

Figure 4

Schematic aid to gene annotations of HRSV whole-genome sequences. An HRSV gene comprises the sequence from the first nucleotide of the conserved HRSV gene start signal (GGGGCAAATa) to the last adenosine residue of the HRSV gene end signal (AGTTAnnnnAAAA) (25,41). Gene start signals are represented by black triangles, and gene end signals are shown as black rectangles, separated by intergenic regions (underlined). Note the M2/L gene overlap (annotations derived from HRSV A2; GenBank accession no. M74568/NC_038235). le, leader region; HRSV, human respiratory syncytial virus; tr, trailer region.

Figure 4. Schematic aid to gene annotations of HRSV whole-genome sequences. An HRSV gene comprises the sequence from the first nucleotide of the conserved HRSV gene start signal (GGGGCAAATa) to the last adenosine residue of the HRSV gene end signal (AGTTAnnnnAAAA) (25,41). Gene start signals are represented by black triangles, and gene end signals are shown as black rectangles, separated by intergenic regions (underlined). Note the M2/L gene overlap (annotations derived from HRSV A2; GenBank accession no. M74568/NC_038235). le, leader region; HRSV, human respiratory syncytial virus; tr, trailer region.

Main Article

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1These authors contributed equally to this article.

2These last authors contributed equally to this article.

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