Affiliation:
1. Department of Microbiology and Molecular Genetics, College of Medicine, University of California, Irvine 92717-4025.
Abstract
The production of poliovirus capsid proteins from a capsid protein precursor (P1) is mediated by virus-encoded proteinase 3CD and involves a complicated set of proteinase-substrate interactions. In addition to substrate and enzymatic determinants required for this interaction, we describe a cellular cofactor, which facilitates 3CD recognition of the P1 precursor. Cellular cofactor activity is 3CD dependent and salt dependent. Our analysis shows that proteolytic cleavage of the P1 precursor at the VP0/VP3 cleavage site exhibits a greater dependency on the cellular cofactor than cleavage at the VP3/VP1 site. Such a greater dependency on cellular cofactor activity can be relieved (in part) by the substitution of an Ala residue for the Pro residue at the -4 position of the VP0/VP3 cleavage site. However, mutant viruses containing Pro-to-Ala substitutions at the -4 position of the VP0/VP3 site exhibit defects in viral growth.
Publisher
American Society for Microbiology
Subject
Virology,Insect Science,Immunology,Microbiology
Reference34 articles.
1. A mutant poliovirus containing a novel proteolytic cleavage site in VP3 is altered in viral maturation;Blair W. S.;J. Virol.,1990
2. Blair W. S. X. Li and B. L. Semler. 3CD cleavage of the poliovirus P1 precursor: a model for complex proteinase/substrate interactions. In L. Carrasco N. Sonenberg and E. Wimmer (ed.) Regulation of gene expression in animal viruses in press. Plenum Press London.
3. .Blair W. S. D. G. Macejak P. Sarnow and B. L. Semler. Unpublished observations.
4. Role for the P4 amino acid residue in substrate utilization by the poliovirus 3CD proteinase;Blair W. S.;J. Virol.,1991
5. .Blair W. S. and B. L. Semler. Unpublished obsevations.
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