Rapid and slow progressors differ by a single MHC class I haplotype in a family of MHC-defined rhesus macaques infected with SIV
Identifieur interne : 003910 ( Main/Exploration ); précédent : 003909; suivant : 003911Rapid and slow progressors differ by a single MHC class I haplotype in a family of MHC-defined rhesus macaques infected with SIV
Auteurs : David T. Evans [États-Unis] ; Leslie A. Knapp [États-Unis] ; Peicheng Jing [États-Unis] ; Jacque L. Mitchen [États-Unis] ; Marta Dykhuizen [États-Unis] ; David C. Montefiori [États-Unis] ; C. David Pauza [États-Unis] ; David I. Watkins [États-Unis]Source :
- Immunology Letters [ 0165-2478 ] ; 1999.
English descriptors
- KwdEn :
- Teeft :
- Aids virus, Allele, Allelic differences, Amino acid sequences, Antibody responses, Assay, Cdna, Cdna bands, Cell line, Ctls, Denaturing gradient, Disease progression, Elsevier science, Epitope, Fresh medium, Generic primers, Haplotype, Heparinized tubes, Heterogeneous virus stock, High neutralizing antibody titers, Immune responses, Immunology, Immunology letters, Important role, Infectious centers assay, Kaslow, Locus, Macaque, Neutralizing, Neutralizing antibody responses, Peptide, Plasma dilution, Plasma virus titers, Pmol primers, Polymorphic, Polymorphic region, Primary viremia, Primer, Progression, Progressors, Rapid progressors, Rhesus, Rhesus macaques, Room temperature, Second round, Sibling, Sibling macaques, Slow progressors, Stable transfectants, Urea gradient, Urea gradients, Variable rates, Viral loads, Viremia, Virus replication.
Abstract
Abstract: Highly polymorphic HLA class I molecules may influence rates of disease progression of HIV-infected individuals. Recent evidence suggests that individuals who mount vigorous CTL responses to multiple HIV-1 epitopes have reduced viral loads, and survive longer than individuals that make a less robust or less diverse CTL response. It has been difficult, however, to define associations between particular HLA class I alleles and rates of disease progression. This may be due, in part, to the uncontrolled variables associated with naturally acquired HIV infections. Studies using MHC-defined, non-human primates infected with well characterized viral stocks should help to clarify this relationship. To explore the possibility that MHC class I polymorphism can influence disease progression, we infected four Mamu-DRB-identical individuals from a family of MHC-defined rhesus macaques intravenously with 40 TCID50SIVmac239. Two of these macaques developed severe wasting and were euthanized within 80 days of infection, while the other two survived for more than 400 days without showing any symptoms of disease. Since all four of these macaques were Mamu-DRB-identical, we were able to exclude the MHC class II DRB loci as determinant of disease progression. Interestingly, both of the slow progressors made CTL responses to the same three SIV CTL epitopes, which were restricted by two molecules (Mamu-B*03 and B*04) encoded by their common maternal haplotype. The two rapid progressors did not share this haplotype with the slow progressors, and we were unable to detect CTL responses in these two siblings. These observations implicate products of the Mamu-B*03 and B*04 alleles in resistance to disease progression in this family of SIV-infected macaques, and provide additional evidence that certain MHC class I-restricted CTL responses may play a significant role in delaying the onset of AIDS.
Url:
DOI: 10.1016/S0165-2478(98)00151-5
Affiliations:
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Recent evidence suggests that individuals who mount vigorous CTL responses to multiple HIV-1 epitopes have reduced viral loads, and survive longer than individuals that make a less robust or less diverse CTL response. It has been difficult, however, to define associations between particular HLA class I alleles and rates of disease progression. This may be due, in part, to the uncontrolled variables associated with naturally acquired HIV infections. Studies using MHC-defined, non-human primates infected with well characterized viral stocks should help to clarify this relationship. To explore the possibility that MHC class I polymorphism can influence disease progression, we infected four Mamu-DRB-identical individuals from a family of MHC-defined rhesus macaques intravenously with 40 TCID50SIVmac239. Two of these macaques developed severe wasting and were euthanized within 80 days of infection, while the other two survived for more than 400 days without showing any symptoms of disease. Since all four of these macaques were Mamu-DRB-identical, we were able to exclude the MHC class II DRB loci as determinant of disease progression. Interestingly, both of the slow progressors made CTL responses to the same three SIV CTL epitopes, which were restricted by two molecules (Mamu-B*03 and B*04) encoded by their common maternal haplotype. The two rapid progressors did not share this haplotype with the slow progressors, and we were unable to detect CTL responses in these two siblings. These observations implicate products of the Mamu-B*03 and B*04 alleles in resistance to disease progression in this family of SIV-infected macaques, and provide additional evidence that certain MHC class I-restricted CTL responses may play a significant role in delaying the onset of AIDS.</div></front></TEI><affiliations><list><country><li>États-Unis</li></country></list><tree><country name="États-Unis"><noRegion><name sortKey="Evans, David T" sort="Evans, David T" uniqKey="Evans D" first="David T." last="Evans">David T. Evans</name></noRegion><name sortKey="Dykhuizen, Marta" sort="Dykhuizen, Marta" uniqKey="Dykhuizen M" first="Marta" last="Dykhuizen">Marta Dykhuizen</name><name sortKey="Jing, Peicheng" sort="Jing, Peicheng" uniqKey="Jing P" first="Peicheng" last="Jing">Peicheng Jing</name><name sortKey="Knapp, Leslie A" sort="Knapp, Leslie A" uniqKey="Knapp L" first="Leslie A." last="Knapp">Leslie A. Knapp</name><name sortKey="Mitchen, Jacque L" sort="Mitchen, Jacque L" uniqKey="Mitchen J" first="Jacque L." last="Mitchen">Jacque L. Mitchen</name><name sortKey="Montefiori, David C" sort="Montefiori, David C" uniqKey="Montefiori D" first="David C." last="Montefiori">David C. Montefiori</name><name sortKey="Pauza, C David" sort="Pauza, C David" uniqKey="Pauza C" first="C. David" last="Pauza">C. David Pauza</name><name sortKey="Watkins, David I" sort="Watkins, David I" uniqKey="Watkins D" first="David I." last="Watkins">David I. Watkins</name><name sortKey="Watkins, David I" sort="Watkins, David I" uniqKey="Watkins D" first="David I." last="Watkins">David I. Watkins</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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