Novel transcription map for the B19 (human) pathogenic parvovirus.

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J Virol. 1987 August; 61(8): 2395-2406

Novel transcription map for the B19 (human) pathogenic parvovirus.

K Ozawa, J Ayub, Y S Hao, G Kurtzman, T Shimada and N Young

ABSTRACT

The B19 parvovirus, a small single-stranded DNA virus of 5.4kilobases, is pathogenic in humans. B19 has remarkable specificityfor erythroid progenitor cells and has been propagated in vitroonly with human erythroid bone marrow. Replication of viralDNA and the viral protein products of B19 appear similar tothose of other animal parvoviruses. However, B19 transcriptionhad unusual features in comparison with that in other animalparvoviruses. At least nine overlapping poly(A)+ transcriptswere identified in infected cells; all but one contained largeintrons. B19 differed from other parvoviruses in the initiationof all transcripts at a strong left side promoter (p6) and theabsence of a functional internal promoter; the presence of short5' leader sequences of about 60 bases and very large intronsfor RNAs encoded by the right side of the genome; two separatetranscription termination sites, in contrast to coterminationat the far right side of the genome for other parvoviruses;the probable utilization by three transcripts of a variant polyadenylationsignal (ATTAAA or AATAAC) in the middle of the genome; and theabundance of two unique transcripts from the middle of the genomewhich did not code for capsid proteins. The unusual transcriptionmap of B19 suggests that regulation of the relative abundanceof transcripts occurs by splicing and termination-polyadenylationevents rather than by promoter strength. In combination withthe published nucleotide sequence, the novel transcription mapseparated the pathogenic B19 virus at a molecular level fromother animal parvoviruses and human adeno-associated virus.

J Virol. 1987 August; 61(8): 2395-2406

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