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Journal of Virology, December 1999, p. 10191-10198, Vol. 73, No. 12
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Efficient Processing of the Immunodominant,
HLA-A*0201-Restricted Human Immunodeficiency Virus Type 1 Cytotoxic
T-Lymphocyte Epitope despite Multiple Variations in the Epitope
Flanking Sequences
Christian
Brander,1,*
Otto O.
Yang,1
Norman G.
Jones,1
Yun
Lee,1
Philip
Goulder,1
R. Paul
Johnson,1,2
Alicja
Trocha,1
David
Colbert,3
Christine
Hay,1
Susan
Buchbinder,3
Cornelia C.
Bergmann,4
Hans J.
Zweerink,5
Steven
Wolinsky,6
William A.
Blattner,7
Spyros A.
Kalams,1 and
Bruce D.
Walker1
AIDS Research Center and Infectious Disease
Unit, Massachusetts General Hospital and Harvard Medical School,
Boston, Massachusetts 021141; New
England Regional Primate Center, Harvard Medical School, Southborough,
Massachusetts 017722; HIV Research
Section, Department of Public Health, San Francisco, California
941023; University of Southern
California School of Medicine, Los Angeles, California
900334; Department of Inflammation
and Rheumatology, Merck Research Laboratories, Rahway, New Jersey
070655; Department of Medicine,
Northwestern University Medical School, Chicago, Illinois
606116; and Division of Geographic
Medicine, University of Maryland, Baltimore, Maryland
212017
Received 26 April 1999/Accepted 29 August 1999
Immune escape from cytotoxic T-lymphocyte (CTL) responses has been
shown to occur not only by changes within the targeted epitope but also
by changes in the flanking sequences which interfere with the
processing of the immunogenic peptide. However, the frequency of such
an escape mechanism has not been determined. To investigate whether
naturally occurring variations in the flanking sequences of an
immunodominant human immunodeficiency virus type 1 (HIV-1) Gag CTL
epitope prevent antigen processing, cells infected with HIV-1 or
vaccinia virus constructs encoding different patient-derived Gag
sequences were tested for recognition by HLA-A*0201-restricted, p17-specific CTL. We found that the immunodominant p17 epitope (SL9)
and its variants were efficiently processed from minigene expressing
vectors and from six HIV-1 Gag variants expressed by recombinant
vaccinia virus constructs. Furthermore, SL9-specific CTL clones derived
from multiple donors efficiently inhibited virus replication when added
to HLA-A*0201-bearing cells infected with primary or laboratory-adapted
strains of virus, despite the variability in the SL9 flanking
sequences. These data suggest that escape from this immunodominant CTL
response is not frequently accomplished by changes in the epitope
flanking sequences.
*
Corresponding author. Mailing address: AIDS Research
Center, Massachusetts General Hospital-East, 149 13th St., Charlestown, MA 02129. Phone: (617) 724-5789. Fax: (617) 726-5411. E-mail: brander{at}helix.mgh.harvard.edu.
Journal of Virology, December 1999, p. 10191-10198, Vol. 73, No. 12
0022-538X/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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