Three different cellular proteins bind to complementary sites on the 5'-end-positive and 3'-end-negative strands of mouse hepatitis virus RNA.

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J Virol. 1993 December; 67(12): 7215-7222

Three different cellular proteins bind to complementary sites on the 5'-end-positive and 3'-end-negative strands of mouse hepatitis virus RNA.

T Furuya and M M Lai

Department of Microbiology, School of Medicine, University of Southern California, Los Angeles 90033-1054.

ABSTRACT

The termini of viral genomic RNA and its complementary strandare important in the initiation of viral RNA replication, whichprobably involves both viral and cellular proteins. To detectthe possible cellular proteins involved in the replication ofmouse hepatitis virus RNA, we performed RNA-protein bindingstudies with RNAs representing both the 5' and 3' ends of theviral genomic RNA and the 3' end of the negative-strand complementaryRNA. Gel-retardation assays showed that both the 5'-end-positive-and 3'-end-negative-strand RNA formed an RNA-protein complexwith cellular proteins from the uninfected cells. UV cross-linkingexperiments further identified a 55-kDa protein bound to the5' end of the positive-strand viral genomic RNA and two proteins35 and 38 kDa in size bound to the 3' end of the negative-strandcRNA. The results of the competition assay confirmed the specificityof this RNA-protein binding. No proteins were found to bindto the 3' end of the viral genomic RNA under the same conditions.The binding site of the 55-kDa protein was mapped within the56-nucleotide region from nucleotides 56 to 112 from the 5'end of the positive-strand RNA, and the 35- and 38-kDa proteinsbound to the complementary region on the negative-strand RNA.The 38-kDa protein was detected only in DBT cells but was notdetected in HeLa or COS cells, while the 35-kDa protein wasfound in all three cell types. The juxtaposition of the differentcellular proteins on the complementary sites near the ends ofthe positive- and negative-strand RNAs suggests that these proteinsmay interact with each other and play a role in mouse hepatitisvirus RNA replication.

J Virol. 1993 December; 67(12): 7215-7222

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