Demographic Processes Affect HIV-1 Evolution in Primary Infection before the Onset of Selective Processes

Herbeck, Joshua T.; Rolland, Morgane; Liu, Y.; McLaughlin, Sherry; McNevin, John; Zhao, Hong; Wong, Kim; Stoddard, Julia N.; Raugi, Dana N.; Sorensen, Stephanie; Genowati, Indira; Birditt, Brian; McKay, A.; Diem, Kurt; Maust, Brandon S.; Deng, Wenjie; Collier, Ann C.; Stekler, Joanne D.; McElrath, M. Juliana; Mullins, James I.

doi:10.1128/jvi.02697-10

Cited by 91 publications

(107 citation statements)

References 76 publications

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“…This observation, coupled with the finding that the proportion of nef codons under negative selection was highest in plasma samples from the same macaques suggests the hypothesis that the emergence of viral strains capable of efficiently invading the CNS may require the fixation of functional Nef capable of altering the macrophage migratory mode. The fixation of nef could also be due to a biological mechanism, such as an early HLA-restricted CTL response, rather than early adaptive viral evolution (64). Further examination of the signatures identified in this study could yield information important for vaccine or therapeutic programs targeting nef.…”

Section: Discussionmentioning

confidence: 99%

Tracking the Emergence of Host-Specific Simian Immunodeficiency Virus env and nef Populations Reveals nef Early Adaptation and Convergent Evolution in Brain of Naturally Progressing Rhesus Macaques

Lamers¹,

Nolan

Rife

et al. 2015

J Virol

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While a clear understanding of the events leading to successful establishment of host-specific viral populations and productive infection in the central nervous system (CNS) has not yet been reached, the simian immunodeficiency virus (SIV)-infected rhesus macaque provides a powerful model for the study of human immunodeficiency virus (HIV) intrahost evolution and neuropathogenesis. The evolution of the gp120 and nef genes, which encode two key proteins required for the establishment and maintenance of infection, was assessed in macaques that were intravenously inoculated with the same viral swarm and allowed to naturally progress to simian AIDS and potential SIV-associated encephalitis (SIVE). Longitudinal plasma samples and immune markers were monitored until terminal illness. Single-genome sequencing was employed to amplify full-length env through nef transcripts from plasma over time and from brain tissues at necropsy. nef sequences diverged from the founder virus faster than gp120 diverged. Host-specific sequence populations were detected in nef (ϳ92 days) before they were detected in gp120 (ϳ182 days). At necropsy, similar brain nef sequences were found in different macaques, indicating convergent evolution, while gp120 brain sequences remained largely host specific. Molecular clock and selection analyses showed weaker clock-like behavior and stronger selection pressure in nef than in gp120, with the strongest nef selection in the macaque with SIVE. Rapid nef diversification, occurring prior to gp120 diversification, indicates that early adaptation of nef in the new host is essential for successful infection. Moreover, the convergent evolution of nef sequences in the CNS suggests a significant role for nef in establishing neurotropic strains. IMPORTANCEThe SIV-infected rhesus macaque model closely resembles HIV-1 immunopathogenesis, neuropathogenesis, and disease progression in humans. Macaques were intravenously infected with identical viral swarms to investigate evolutionary patterns in the gp120 and nef genes leading to the emergence of host-specific viral populations and potentially linked to disease progression. Although each macaque exhibited unique immune profiles, macaque-specific nef sequences evolving under selection were consistently detected in plasma samples at 3 months postinfection, significantly earlier than in gp120 macaque-specific sequences. On the other hand, nef sequences in brain tissues, collected at necropsy of two animals with detectable infection in the central nervous system (CNS), revealed convergent evolution. The results not only indicate that early adaptation of nef in the new host may be essential for successful infection, but also suggest that specific nef variants may be required for SIV to efficiently invade CNS macrophages and/or enhance macrophage migration, resulting in HIV neuropathology. Aclear understanding of the events leading to the establishment of human immunodeficiency virus type 1 (HIV-1) infection in a new host, including the central nervous system (C...

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Section: Discussionmentioning

confidence: 99%

Tracking the Emergence of Host-Specific Simian Immunodeficiency Virus env and nef Populations Reveals nef Early Adaptation and Convergent Evolution in Brain of Naturally Progressing Rhesus Macaques

Lamers¹,

Nolan

Rife

et al. 2015

J Virol

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“…25,36 Vif and Vpr, but not Vpu, have low entropy in t/f viruses To investigate HIV-1C Vif, Vpr, and Vpr amino acid diversity, we reconstructed each patient's t/f virus, using the consensus sequence from the earliest time point postinfection, and computed Shannon entropy scores across Vif, Vpr, and Vpu t/f alignments. The median number of sequences per patient used for reconstruction was 10 [interquartile range [(IQR): [5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20][21][22][23][24]. The reconstructed t/f viruses exhibited relatively low interpatient amino acid entropy in Vif (median 0.00; IQR: 0.00-0.22) and Vpr (median 0.00; IQR: 0.00-0.22) (Fig.…”

Section: Clinical Characteristics and Interpatient Viral Quasispeciesmentioning

confidence: 99%

“…Following this, cytotoxic T lymphocytes (CTLs) play a critical role in the control of HIV infection and mediate another bottleneck event from which escape variants emerge. 11 Human leukocyte antigen (HLA) class I-mediated CTL responses are important predictors of disease progression 12 that drive virus escape mutations that are highly adapted to the host environment. 4,[13][14][15][16][17][18] Recent studies employing ultradeep sequencing 3,19 confirmed dramatic shifts in the frequencies of epitope variants during the first weeks of HIV infection.…”

Section: Introductionmentioning

confidence: 99%

Transmitted/Founder HIV-1 Subtype C Viruses Show Distinctive Signature Patterns in Vif, Vpr, and Vpu That Are Under Subsequent Immune Pressure During Early Infection

Rossenkhan

MacLeod

Brumme

et al. 2016

AIDS Research and Human Retroviruses

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Viral variants that predominate during early infection may exhibit constrained diversity compared with those found during chronic infection and could contain amino acid signature patterns that may enhance transmission, establish productive infection, and influence early events that modulate the infection course. We compared amino acid distributions in 17 patients recently infected with HIV-1C with patients with chronic infection. We found significantly lower entropy in inferred transmitted/founder (t/f) compared with chronic viruses and identified signature patterns in Vif and Vpr from inferred t/f viruses. We investigated sequence evolution longitudinally up to 500 days postseroconversion and compared the impact of selected substitutions on predicted human leukocyte antigen (HLA) binding affinities of published and predicted cytotoxic T-lymphocyte epitopes. Polymorphisms in Vif and Vpr during early infection occurred more frequently at epitope-HLA anchor residues and significantly decreased predicted epitope-HLA binding. Transmission-associated sequence signatures may have implications for novel strategies to prevent HIV-1 transmission.

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“…However, in many responses detected during primary HIV-1 infection, clear evidence of reversions is difficult to determine and escape pathways are less consistent (5,11,30). Interestingly, frequent sampling of viral populations during acute infection revealed that escape processes can be highly dynamic, with multiple simultaneous or rapidly sequential and mutually exclusive escape mutations arising within a targeted epitope (5). It is unclear which selective forces promote these dynamic escape processes and why some variants are selected over others.…”

mentioning

confidence: 99%

“…These responses consistently promote dominant escape and reversion pathways in which only a select few mutations are required (27)(28)(29). However, in many responses detected during primary HIV-1 infection, clear evidence of reversions is difficult to determine and escape pathways are less consistent (5,11,30). Interestingly, frequent sampling of viral populations during acute infection revealed that escape processes can be highly dynamic, with multiple simultaneous or rapidly sequential and mutually exclusive escape mutations arising within a targeted epitope (5).…”

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confidence: 99%

Fitness-Balanced Escape Determines Resolution of Dynamic Founder Virus Escape Processes in HIV-1 Infection

Sunshine

Larsen

Maust

et al. 2015

J Virol

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To understand the interplay between host cytotoxic T-lymphocyte (CTL) responses and the mechanisms by which HIV-1 evades them, we studied viral evolutionary patterns associated with host CTL responses in six linked transmission pairs. HIV-1 sequences corresponding to full-length p17 and p24 gag were generated by 454 pyrosequencing for all pairs near the time of transmission, and seroconverting partners were followed for a median of 847 days postinfection. T-cell responses were screened by gamma interferon/interleukin-2 (IFN-␥/IL-2) FluoroSpot using autologous peptide sets reflecting any Gag variant present in at least 5% of sequence reads in the individual's viral population. While we found little evidence for the occurrence of CTL reversions, CTL escape processes were found to be highly dynamic, with multiple epitope variants emerging simultaneously. We found a correlation between epitope entropy and the number of epitope variants per response (r ‫؍‬ 0.43; P ‫؍‬ 0.05). In cases in which multiple escape mutations developed within a targeted epitope, a variant with no fitness cost became fixed in the viral population. When multiple mutations within an epitope achieved fitness-balanced escape, these escape mutants were each maintained in the viral population. Additional mutations found to confer escape but undetected in viral populations incurred high fitness costs, suggesting that functional constraints limit the available sites tolerable to escape mutations. These results further our understanding of the impact of CTL escape and reversion from the founder virus in HIV infection and contribute to the identification of immunogenic Gag regions most vulnerable to a targeted T-cell attack. IMPORTANCERapid diversification of the viral population is a hallmark of HIV-1 infection, and understanding the selective forces driving the emergence of viral variants can provide critical insight into the interplay between host immune responses and viral evolution. We used deep sequencing to comprehensively follow viral evolution over time in six linked HIV transmission pairs. We then mapped T-cell responses to explore if mutations arose due to adaption to the host and found that escape processes were often highly dynamic, with multiple mutations arising within targeted epitopes. When we explored the impact of these mutations on replicative capacity, we found that dynamic escape processes only resolve with the selection of mutations that conferred escape with no fitness cost to the virus. These results provide further understanding of the complicated viral-host interactions that occur during early HIV-1 infection and may help inform the design of future vaccine immunogens. Exploring the dynamic interplay between human immune responses and the mechanisms by which HIV-1 evades these responses can help inform which types and specificity of immunity a vaccine should elicit. At peak viral load, the viral population is usually homogenous (1-3). In approximately 75% of HIV transmissions, a single variant (the "founder" virus) es...

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Demographic Processes Affect HIV-1 Evolution in Primary Infection before the Onset of Selective Processes

Cited by 91 publications

References 76 publications

Tracking the Emergence of Host-Specific Simian Immunodeficiency Virus env and nef Populations Reveals nef Early Adaptation and Convergent Evolution in Brain of Naturally Progressing Rhesus Macaques

Tracking the Emergence of Host-Specific Simian Immunodeficiency Virus env and nef Populations Reveals nef Early Adaptation and Convergent Evolution in Brain of Naturally Progressing Rhesus Macaques

Transmitted/Founder HIV-1 Subtype C Viruses Show Distinctive Signature Patterns in Vif, Vpr, and Vpu That Are Under Subsequent Immune Pressure During Early Infection

Fitness-Balanced Escape Determines Resolution of Dynamic Founder Virus Escape Processes in HIV-1 Infection

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