4.7 Article

Macaques vaccinated with live-attenuated SIV control replication of heterologous virus

Journal

JOURNAL OF EXPERIMENTAL MEDICINE
Volume 205, Issue 11, Pages 2537-2550

Publisher

ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20081524

Keywords

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Funding

  1. International AIDS Vaccine Initiative
  2. National Institutes of Health [R01 AI049120, R01 AI052056]
  3. National Center for Research Resources [P51 RR000167]
  4. National Institutes of Health
  5. Research Facilities Improvement Program [RR15459-01, RR020141-01]
  6. Medical Research Council (UK)
  7. MRC [G0501963] Funding Source: UKRI
  8. Medical Research Council [G0501963] Funding Source: researchfish

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An effective AIDS vaccine will need to protect against globally diverse isolates of HIV. To address this issue in macaques, we administered a live-attenuated simian immunodeficiency virus (SIV) vaccine and challenged with a highly pathogenic heterologous isolate. Vaccinees reduced viral replication by similar to 2 logs between weeks 2-32 (P <= 0.049) postchallenge. Remarkably, vaccinees expressing MHC-I (MHC class I) alleles previously associated with viral control completely suppressed acute phase replication of the challenge virus, implicating CD8(+) T cells in this control. Furthermore, transient depletion of peripheral CD8(+) lymphocytes in four vaccinees during the chronic phase resulted in an increase in virus replication. In two of these animals, the recrudescent virus population contained only the vaccine strain and not the challenge virus. Alarmingly, however, we found evidence of recombinant viruses emerging in some of the vaccinated animals. This finding argues strongly against an attenuated virus vaccine as a solution to the AIDS epidemic. On a more positive note, our results suggest that MHC-I-restricted CD8(+) T cells contribute to the protection induced by the live-attenuated SIV vaccine and demonstrate that vaccine-induced CD8(+) T cell responses can control replication of heterologous challenge viruses.

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