TY - JOUR
T1 - Broad CTL response is required to clear latent HIV-1 due to dominance of escape mutations
AU - Deng, Kai
AU - Pertea, Mihaela
AU - Rongvaux, Anthony
AU - Wang, Leyao
AU - Durand, Christine M.
AU - Ghiaur, Gabriel
AU - Lai, Jun
AU - McHugh, Holly L.
AU - Hao, Haiping
AU - Zhang, Hao
AU - Margolick, Joseph B.
AU - Gurer, Cagan
AU - Murphy, Andrew J.
AU - Valenzuela, David M.
AU - Yancopoulos, George D.
AU - Deeks, Steven G.
AU - Strowig, Till
AU - Kumar, Priti
AU - Siliciano, Janet D.
AU - Salzberg, Steven L.
AU - Flavell, Richard A.
AU - Shan, Liang
AU - Siliciano, Robert F.
N1 - Publisher Copyright:
© 2015 Macmillan Publishers Limited.
PY - 2015/1/15
Y1 - 2015/1/15
N2 - Despite antiretroviral therapy (ART),humanimmunodeficiency virus (HIV)-1 persists in a stable latent reservoir1,2, primarily in resting memory CD41 T cells3,4. This reservoir presents a major barrier to the cure of HIV-1 infection. To purge the reservoir, pharmacological reactivation of latent HIV-1 has been proposed5 and tested both in vitro and in vivo6-8. A key remaining question is whether virusspecific immune mechanisms, including cytotoxic T lymphocytes (CTLs), can clear infected cells in ART-treated patients after latency is reversed. Here we show that there is a striking all or none pattern for CTL escape mutations in HIV-1 Gag epitopes. Unless ART is started early, the vast majority (.98%) of latent viruses carry CTL escapemutations that render infectedcells insensitive toCTLsdirected at common epitopes. To solve this problem, we identified CTLs that could recognize epitopes fromlatent HIV-1 that were unmutated in every chronically infected patient tested. Upon stimulation, these CTLs eliminated target cells infected with autologous virus derived fromthe latent reservoir, bothinvitro andinpatient-derived humanized mice. The predominance of CTL-resistant viruses in the latent reservoir poses a major challenge to viral eradication. Our results demonstrate that chronically infected patients retain a broad-spectrum viral-specific CTL response and that appropriate boosting of this response may be required for the elimination of the latent reservoir.
AB - Despite antiretroviral therapy (ART),humanimmunodeficiency virus (HIV)-1 persists in a stable latent reservoir1,2, primarily in resting memory CD41 T cells3,4. This reservoir presents a major barrier to the cure of HIV-1 infection. To purge the reservoir, pharmacological reactivation of latent HIV-1 has been proposed5 and tested both in vitro and in vivo6-8. A key remaining question is whether virusspecific immune mechanisms, including cytotoxic T lymphocytes (CTLs), can clear infected cells in ART-treated patients after latency is reversed. Here we show that there is a striking all or none pattern for CTL escape mutations in HIV-1 Gag epitopes. Unless ART is started early, the vast majority (.98%) of latent viruses carry CTL escapemutations that render infectedcells insensitive toCTLsdirected at common epitopes. To solve this problem, we identified CTLs that could recognize epitopes fromlatent HIV-1 that were unmutated in every chronically infected patient tested. Upon stimulation, these CTLs eliminated target cells infected with autologous virus derived fromthe latent reservoir, bothinvitro andinpatient-derived humanized mice. The predominance of CTL-resistant viruses in the latent reservoir poses a major challenge to viral eradication. Our results demonstrate that chronically infected patients retain a broad-spectrum viral-specific CTL response and that appropriate boosting of this response may be required for the elimination of the latent reservoir.
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U2 - 10.1038/nature14053
DO - 10.1038/nature14053
M3 - Article
C2 - 25561180
AN - SCOPUS:84922764937
SN - 0028-0836
VL - 517
SP - 381
EP - 385
JO - Nature
JF - Nature
IS - 7534
ER -