HIV-1 superinfection despite broad CD8+ T-cell responses containing replication of the primary virus

被引:0
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作者
Marcus Altfeld
Todd M. Allen
Xu G. Yu
Mary N. Johnston
Deepak Agrawal
Bette T. Korber
David C. Montefiori
David H. O'Connor
Ben T. Davis
Paul K. Lee
Erica L. Maier
Jason Harlow
Philip J. R. Goulder
Christian Brander
Eric S. Rosenberg
Bruce D. Walker
机构
[1] Harvard Medical School,Partners AIDS Research Center and Infectious Disease Division, Massachusetts General Hospital and Division of AIDS
[2] Los Alamos National Laboratory,Department of Surgery
[3] Duke University Medical Center,Wisconsin Regional Primate Research Center
[4] University of Wisconsin,undefined
[5] Department of Pediatrics,undefined
[6] Nuffield Department of Medicine,undefined
[7] Peter Medawar Building for Pathogen Research,undefined
来源
Nature | 2002年 / 420卷
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摘要
Early treatment of acute HIV-1 infection followed by treatment interruptions has shown promise for enhancing immune control of infection1,2,3. A subsequent loss of control, however, allows the correlates of protective immunity to be assessed. Here we show that sudden breakthrough of plasma viraemia occurred after prolonged immune containment in an individual infected with HIV-1 at a time when 25 distinct CD8+ T-cell epitopes in the viral proteins Gag, RT, Integrase, Env, Nef, Vpr, Vif and Rev were being targeted. Sequencing of the virus in plasma and cells showed that superinfection with a second clade-B virus was coincident with the loss of immune control. This sudden increase in viraemia was associated with a decline in half of the CD8+ T-cell responses. The declining CD8+ T-cell responses were coupled with sequence changes relative to the initial virus that resulted in impaired recognition. Our data show that HIV-1 superinfection can occur in the setting of a strong and broadly directed virus-specific CD8+ T-cell response. The lack of cross-protective immunity for closely related HIV-1 strains, despite persistent recognition of multiple CD8 epitopes, has important implications for public health and vaccine development.
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页码:434 / 439
页数:5
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