Binding of Cellular P32 Protein to the Rubella Virus P150 Replicase Protein Via PxxPxR Motifs

Overview

Journal J Gen Virol

Specialty Microbiology

Date 2012 Jan 13

PMID 22238231

Citations 3

Authors

Suganthi Suppiah

Heather A Mousa

Wen-Pin Tzeng

Jason D Matthews

Teryl K Frey

Affiliations

Soon will be listed here.

Abstract

A proline-rich region (PRR) within the rubella virus (RUBV) P150 replicase protein that contains three SH3 domain-binding motifs (PxxPxR) was investigated for its ability to bind cell proteins. Pull-down experiments using a glutathione S-transferase-PRR fusion revealed PxxPxR motif-specific binding with human p32 protein (gC1qR), which could be mediated by either of the first two motifs. This finding was of interest because p32 protein also binds to the RUBV capsid protein. Binding of p32 to P150 was confirmed and was abolished by mutation of the first two motifs. When mutations in the first two motifs were introduced into a RUBV cDNA infectious clone, virus replication was significantly impaired. However, virus RNA synthesis was found to be unaffected, and subsequent immunofluorescence analysis of RUBV-infected cells revealed co-localization of p32 and P150 but little overlap of p32 with RNA replication complexes, indicating that p32 does not participate directly in virus RNA synthesis. Thus, the role of p32 in RUBV replication remains unresolved.

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