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Attenuation of replication by a 29 nucleotide deletion in SARS-coronavirus acquired during the early stages of human-to-human transmission

Authors :
Muth, Doreen
Corman, Victor Max
Roth, Hanna
Binger, Tabea
Dijkman, Ronald
Gottula, Lina Theresa
Gloza-Rausch, Florian
Balboni, Andrea
Battilani, Mara
Rihtarič, Danijela
Toplak, Ivan
Ameneiros, Ramón Seage
Pfeifer, Alexander
Thiel, Volker
Drexler, Jan Felix
Müller, Marcel Alexander
Drosten, Christian
Muth D, Corman VM, Roth H, Binger T, Dijkman R, Gottula LT, Gloza-Rausch F, Balboni A, Battilani M, Rihtarič D, Toplak I, Ameneiros RS, Pfeifer A, Thiel V, Drexler JF, Müller MA, Drosten C
Source :
Scientific Reports, Scientific Reports, Vol 8, Iss 1, Pp 1-11 (2018), Muth, Doreen; Corman, Victor Max; Roth, Hanna; Binger, Tabea; Dijkman, Ronald; Gottula, Lina Theresa; Gloza-Rausch, Florian; Balboni, Andrea; Battilani, Mara; Rihtarič, Danijela; Toplak, Ivan; Ameneiros, Ramón Seage; Pfeifer, Alexander; Thiel, Volker Earl; Drexler, Jan Felix; Müller, Marcel Alexander; Drosten, Christian (2018). Attenuation of replication by a 29 nucleotide deletion in SARS-coronavirus acquired during the early stages of human-to-human transmission. Scientific Reports, 8(1), p. 15177. Nature Publishing Group 10.1038/s41598-018-33487-8
Publication Year :
2018

Abstract

A 29 nucleotide deletion in open reading frame 8 (ORF8) is the most obvious genetic change in severe acute respiratory syndrome coronavirus (SARS-CoV) during its emergence in humans. In spite of intense study, it remains unclear whether the deletion actually reflects adaptation to humans. Here we engineered full, partially deleted (−29 nt), and fully deleted ORF8 into a SARS-CoV infectious cDNA clone, strain Frankfurt-1. Replication of the resulting viruses was compared in primate cell cultures as well as Rhinolophus bat cells made permissive for SARS-CoV replication by lentiviral transduction of the human angiotensin-converting enzyme 2 receptor. Cells from cotton rat, goat, and sheep provided control scenarios that represent host systems in which SARS-CoV is neither endemic nor epidemic. Independent of the cell system, the truncation of ORF8 (29 nt deletion) decreased replication up to 23-fold. The effect was independent of the type I interferon response. The 29 nt deletion in SARS-CoV is a deleterious mutation acquired along the initial human-to-human transmission chain. The resulting loss of fitness may be due to a founder effect, which has rarely been documented in processes of viral emergence. These results have important implications for the retrospective assessment of the threat posed by SARS.

Details

ISSN :
20452322
Volume :
8
Issue :
1
Database :
OpenAIRE
Journal :
Scientific reports
Accession number :
edsair.doi.dedup.....bb50c98b7334bab68b434be8bf740025