๐ Exceptional flexibility in the sequence requirements for coronavirus small envelope protein function
The small envelope protein (E) plays a role of central importance in the assembly of coronaviruses. This was initially established by studies demonstrating that cellular expression of only E protein and the membrane protein (M) was necessary and sufficient for the generation and release of virus-like particles. To investigate the role of E protein in the whole virus, we previously generated E gene mutants of mouse hepatitis virus (MHV) that were defective in viral growth and produced aberrantly assembled virions. Surprisingly, however, we were also able to isolate a viable MHV mutant (ฮE) in which the entire E gene, as well as the nonessential upstream genes 4 and 5a, were deleted. We have now constructed an E knockout mutant that confirms that the highly defective phenotype of the ฮE mutant is due to loss of the E gene. Additionally, we have created substitution mutants in which the MHV E gene was replaced by heterologous E genes from viruses spanning all three groups of the coronavirus family. Group 2 and 3 E proteins were readily exchangeable for that of MHV. However, the E protein of a group 1 coronavirus, transmissible gastroenteritis virus, became functional in MHV only after acquisition of particular mutations. Our results show that proteins encompassing a remarkably diverse range of primary amino acid sequences can provide E protein function in MHV. These findings suggest that E protein facilitates viral assembly in a manner that does not require E protein to make sequence-specific contacts with M protein. Copyright ยฉ 2007, American Society for Microbiology.
keywords
๐ hepatitis virus (437)
๐ acid sequence (108)
๐ amino acid (454)
๐ acid sequences (44)
๐ mouse hepatitis (371)
๐ gastroenteritis virus (188)
๐ membrane protein (93)
๐ findings suggest (77)
๐ transmissible gastroenteritis (226)
year
โฐ 2007
journal
๐ Journal of Virology
issn
๐ 0022538X
volume
81
number
5
page
2249-2262
citedbycount
31
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