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Journal of Virology, March 1999, p. 1802-1808, Vol. 73, No. 3
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
The Hypervariable Domain of the Murine Leukemia
Virus Surface Protein Tolerates Large Insertions and Deletions,
Enabling Development of a Retroviral Particle Display
System
Samuel C.
Kayman,*
Han
Park,
Maya
Saxon, and
Abraham
Pinter
Laboratory of Retroviral Biology, Public
Health Research Institute, New York, New York 10016
Received 9 September 1998/Accepted 4 December 1998
The surface proteins (SU) of murine type-C retroviruses have a
central hypervariable domain devoid of cysteine and rich in proline.
This 41-amino-acid region of Friend ecotropic murine leukemia virus SU
was shown to be highly tolerant of insertions and deletions. Viruses in
which either the N-terminal 30 amino acids or the C-terminal 22 amino
acids of this region were replaced by the 7-amino-acid sequence ASAVAGA
were fully infectious. Insertions of this 7-amino-acid sequence at the
N terminus, center, and the C terminus of the hypervariable domain had
little effect on envelope protein (Env) function, while this insertion
at a position 10 amino acids following the N terminus partially
destabilized the association between the SU and transmembrane subunits
of Env. Large, complex domains (either a 252-amino-acid single-chain
antibody binding domain [scFv] or a 96-amino-acid V1/V2 domain of
HIV-1 SU containing eight N-linked glycosylation sites and two
disulfides) did not interfere with Env function when inserted in the
center or C-terminal portions of the hypervariable domain. The scFv
domain inserted into the C-terminal region of the hypervariable domain was shown to mediate binding of antigen to viral particles,
demonstrating that it folded into the active conformation and was
displayed on the surface of the virion. Both positive and negative
enrichment of virions expressing the V1/V2 sequence were achieved by
using a monoclonal antibody specific for a conformational epitope
presented by the inserted sequence. These results indicated that the
hypervariable domain of Friend ecotropic SU does not contain any
specific sequence or structure that is essential for Env function and
demonstrated that insertions into this domain can be used to extend
particle display methodologies to complex protein domains that require expression in eukaryotic cells for glycosylation and proper folding.
*
Corresponding author. Mailing address: Laboratory of
Retroviral Biology, Public Health Research Institute, 455 First Ave., New York, NY 10016. Phone: (212) 576-8432. Fax: (212) 578-0804. E-mail: skayman{at}phri.nyu.edu.
Journal of Virology, March 1999, p. 1802-1808, Vol. 73, No. 3
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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