Nucleotide sequencing of an apparent proviral copy of env mRNA defines determinants of expression of the mouse mammary tumor virus env gene

Author:

Majors J E,Varmus H E

Abstract

To extend our understanding of the organization and expression of the mouse mammary tumor virus genome, we determined the nucleotide sequence of large regions of a cloned mouse mammary tumor virus strain C3H provirus that appears to be a DNA copy of env mRNA. In conjunction with analysis of several additional clones of integrated and unintegrated mouse mammary tumor virus DNAs, we came to the following conclusions: (i) the mRNA for env is generated by splicing mechanisms that recognize conventional eucaryotic signals at donor and acceptor sites with a leader of at least 289 bases in length; (ii) the first of three possible initiation codons for translation of env follows the splice junction by a single nucleotide and produces a signal peptide of 98 amino acids; (iii) the amino terminal sequence of the major virion glycoprotein gp52env is confirmed by nucleotide sequencing and is encoded by a sequence beginning 584 nucleotides from the 5' end of env mRNA; (iv) the final 17 amino acids at the carboxyl terminus of the primary product of env are encoded within the long terminal repeat by the 51 bases at the 5' end of the U3 domain; and (v) bases 2 through 4 at the 5' end of the long terminal repeat constitute an initiation codon that commences an open reading frame capable of directing the synthesis of a 36-kilodalton protein.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

Reference32 articles.

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2. Processing and amino acid sequence analysis of the mouse mammary tumor virus env gene product;Arthur L. O.;J. Virol.,1982

3. Structure and processing of the mouse mammary tumor virus glycoprotein precursor Pr 73e"n;Dickson C.;J. Virol.,1980

4. Dickson C. R. Eisenman H. Fan E. Hunter and N. Teich. 1982. In R. Weiss N. Teich H. Varmus and J. Coffin (ed.) Molecular biology of tumor viruses. Part III. RNA tumor viruses p. 513-648. Cold Spring Harbor Laboratory Cold Spring Harbor N.Y.

5. Protein-coding potential of mouse mammary tumor virus genome RNA as examined by in vitro translation;Dickson C.;J. Virol.,1981

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