Broad CTL response is required to clear latent HIV-1 due to dominance of escape mutations

Deng, Kai; Pertea, Mihaela; Rongvaux, Anthony; Wang, Leyao; Durand, Christine M.; Ghiaur, Gabriel; Lai, Jun; McHugh, Holly; Hao, Haiping; Zhang, Hao; Margolick, Joseph B.; Gurer, Cagan; Murphy, Andrew J.; Valenzuela, David M.; Yancopouloš, George D.; Deeks, Steven G.; Strowig, Till; Kumar, Priti; Siliciano, Janet D.; Salzberg, Steven L.; Flavell, Richard A.; Shan, Liang; Siliciano, Robert F.

doi:10.1038/nature14053

Cited by 449 publications

(452 citation statements)

References 34 publications

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“…[7][8][9][10][11] Because residual HIV expression continues despite effective ART [12][13][14][15][16] and is required for viral rebound, HIV-infected cells should theoretically be targetable by a T cell therapeutic agent. Several mechanisms are thought to be responsible for the apparent failure of autologous cytotoxic T lymphocytes (CTLs) to clear reactivated cells in HIV-infected individuals: HIV evolution prior to ART quickly selects for CTL escape mutations; [17][18][19] HIV Nef mediates downregulation of major histocompatibility complex class I (MHC-I), 20,21 protecting HIV-infected cells from T cell receptor (TCR)-dependent CTL killing; and HIV-specific CTL responses may be limited by exhaustion 22,23 or peripheral immune tolerance. 24,25 Over the last decade, major advances have been made in engineering human T cells via introduction of chimeric antigen receptors (CARs) to enable specific lysis of pathogenic targets.…”

Section: Introductionmentioning

confidence: 99%

Engineering HIV-Resistant, Anti-HIV Chimeric Antigen Receptor T Cells

Hale¹,

Mesojednik

Ibarra³

et al. 2017

Molecular Therapy

139

154

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Section: Introductionmentioning

confidence: 99%

Engineering HIV-Resistant, Anti-HIV Chimeric Antigen Receptor T Cells

Hale¹,

Mesojednik

Ibarra³

et al. 2017

Molecular Therapy

139

154

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“…12 Early treatment also prevents the latent viral reservoir from becoming dominated by HIV-1 variants that have mutated to escape cytotoxic T lymphocytes (CTL); this has implications for both therapeutic vaccine design and HIV cure strategies. 13 Furthermore, earlier initiation of cART and higher nadir CD4 T-cell counts have been associated with the preservation of functional recall T-cell responses.…”

Section: Early Initiation Of Cart Facilitates Efficacious Immunotheramentioning

confidence: 99%

“…However, immunization in conjunction with cART may lead to a reversal of anergy by selective induction and activation of specific memory T-cell responses against a number of viral proteins. 3,20 By presenting viral proteins in novel ways, with or without specific adjuvants, or by presenting both immunodominant and subdominant epitopes, specific beneficial memory responses may be induced or augmented, 13 and T-cell anergy reversed. That said, even administered in the context of cART, therapeutic immunization is likely to have little efficacy if used without other concomitant immunotherapies due to the immunocompromised status of chronically HIV-1-infected patients.…”

Section: Essential Role Of Therapeutic Vaccines To Provide Antigenicmentioning

confidence: 99%

“…57 The vast majority of viruses in the latent reservoir of patients treated during chronic HIV-1 infection comprise CTL escape mutations, which are rare in the reservoirs of subjects treated during acute infection. 13 Recent work shows that only 12% of proviruses are non-mutated and replication competent. 58 However, measurement of HIV-1 latency reversal ex vivo using a different approach revealed that only 1.5% of proviruses in resting CD4 T cells were able to produce virions following CD3/ CD28 activation.…”

Section: Proviral Dna and Quantification Of Replication-competent Virusmentioning

confidence: 99%

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Multifarious immunotherapeutic approaches to cure HIV-1 infection

Imami

Herasimtschuk

2015

Human Vaccines & Immunotherapeutics

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“…It has been suggested that variable sequences can serve as immunodominant “decoys” that can absorb immune reactivity, driving the emergence of escape mutations and potentially precluding responses against conserved protective epitopes. 29–35 The mechanisms of this preclusion, also referred to as immunodomination, 36 are varied. 37 , 38 Virus-specific T cells are responsible for controlling viremia in humans and macaques.…”

Section: Introductionmentioning

confidence: 99%

Gag and env conserved element CE DNA vaccines elicit broad cytotoxic T cell responses targeting subdominant epitopes of HIV and SIV Able to recognize virus-infected cells in macaques

Valentı́n

et al. 2018

Human Vaccines & Immunotherapeutics

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HIV sequence diversity and the propensity of eliciting immunodominant responses targeting inessential variable regions are hurdles in the development of an effective AIDS vaccine. We developed a DNA vaccine comprising conserved elements (CE) of SIV p27Gag and HIV-1 Env and found that priming vaccination with CE DNA is critical to efficiently overcome the dominance imposed by Gag and Env variable regions. Here, we show that DNA vaccinated macaques receiving the CE prime/CE+full-length DNA co-delivery booster vaccine regimens developed broad, potent and durable cytotoxic T cell responses targeting conserved protein segments of SIV Gag and HIV Env. Gag CE-specific T cells showed robust anamnestic responses upon infection with SIVmac239 which led to the identification of CE-specific cytotoxic lymphocytes able to recognize epitopes covering distinct CE on the surface of SIV infected cells in vivo. Though not controlling infection overall, we found an inverse correlation between Gag CE-specific CD8+ T cell responses and peak viremia. The T cell responses induced by the HIV Env CE immunogen were recalled in some animals upon SIV infection, leading to the identification of two cross-reactive epitopes between HIV and SIV Env based in sequence homology. These data demonstrate that a vaccine combining Gag and Env CE DNA subverted the normal immunodominance patterns, eliciting immune responses that included subdominant, highly conserved epitopes. These vaccine regimens augment cytotoxic T cell responses to highly conserved epitopes in the viral proteome and maximize response breadth. The vaccine-induced CE-specific T cells were expanded upon SIV infection, indicating that the predicted CE epitopes incorporated in the DNA vaccine are processed and exposed by infected cells in their natural context within the viral proteome.

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Broad CTL response is required to clear latent HIV-1 due to dominance of escape mutations

Cited by 449 publications

References 34 publications

Engineering HIV-Resistant, Anti-HIV Chimeric Antigen Receptor T Cells

Engineering HIV-Resistant, Anti-HIV Chimeric Antigen Receptor T Cells

Multifarious immunotherapeutic approaches to cure HIV-1 infection

Gag and env conserved element CE DNA vaccines elicit broad cytotoxic T cell responses targeting subdominant epitopes of HIV and SIV Able to recognize virus-infected cells in macaques

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