Reverse transcription of retroviral genomes: mutations in the terminal repeat sequences.

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J Virol. 1985 February; 53(2): 447-455

Reverse transcription of retroviral genomes: mutations in the terminal repeat sequences.

L I Lobel and S P Goff

ABSTRACT

The process of reverse transcription of retroviral genomes beginswith the synthesis of a short DNA molecule near the 5' end ofthe RNA template. This molecule, termed minus-strand strong-stopDNA, is then translocated to the 3' end of the viral RNA bymeans of a repeated sequence, the R region, present at bothends of the template. The translocation should result in thetransfer of genetic information from the 5' R region to the3' R region. We have generated a series of mutants of Moloneymurine leukemia virus with alterations in the R regions by invitro mutagenesis of a cloned DNA copy of the viral genome.The altered DNAs were introduced into mouse cells by transfection,and the translocation of the mutations during viral replicationwas assessed. Some mutations were not transferred from the 5'R region to the 3' R region; these results were not in accordwith current models for reverse transcription. The results canbe explained if DNA molecules shorter than strong-stop DNA,formed by premature termination of synthesis, are sometimestranslocated. A number of mutants with large deletions in theR region were tested and were able to replicate with normalstrong-stop DNA translocation. Thus, short stretches of homologycan be used by the virus to carry out strong-stop translocations.

J Virol. 1985 February; 53(2): 447-455

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