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Journal of Virology, December 2000, p. 11511-11521, Vol. 74, No. 24
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Efficient Replication of Adeno-Associated Virus Type 2 Vectors: a cis-Acting Element outside of the
Terminal Repeats and a Minimal Size
Gregory E.
Tullis
and
Thomas
Shenk*
Department of Molecular Biology, Princeton
University, Princeton, New Jersey 08544-1014
Received 31 July 2000/Accepted 25 September 2000
Recombinant adeno-associated virus type 2 (AAV2) can be produced in
adenovirus-infected cells by cotransfecting a plasmid containing the
recombinant AAV2 genome, which is generally comprised of the viral
terminal repeats flanking a transgene, together with a second plasmid
expressing the AAV2 rep and cap genes. However, recombinant viruses generally replicate inefficiently, often producing 100-fold fewer virus particles per cell than can be obtained after transfection with a plasmid containing a wild-type AAV2 genome. We
demonstrate that this defect is due, at least in part, to the presence
of a positive-acting cis element between nucleotides 194 and 1882 of AAV2. Recombinant AAV2 genomes lacking this region accumulated 14-fold less double-stranded, monomer-length
replicative-form DNA than did wild-type AAV2. In addition, we
demonstrate that a minimum genome size of 3.5 kb is required for
efficient production of single-stranded viral DNA. Relatively small
recombinant genomes (2,992 and 3,445 bp) accumulated three- to
eightfold less single-stranded DNA per monomer-length replicative-form
DNA molecule than wild-type AAV2. In contrast, recombinant AAV2 with
larger genomes (3,555 to 4,712 bp) accumulated similar amounts of
single-stranded DNA per monomer-length replicative-form DNA compared to
wild-type AAV2. Analysis of two recombinant AAV2 genomes less than 3.5 kb in size indicated that they were deficient in the production of the
extended form of monomer-length replicative-form DNA, which is thought
to be the immediate precursor to single-stranded AAV2 DNA.
*
Corresponding author. Mailing address: Department of
Molecular Biology, Princeton University, Princeton, NJ 08544-1014. Phone: (609) 258-5992. Fax: (609) 258-1704. E-mail:
tshenk{at}princeton.edu.

Present address: Avigen, Inc., Alameda, CA
94501.
Journal of Virology, December 2000, p. 11511-11521, Vol. 74, No. 24
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
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