2020
DOI: 10.1016/j.xcrm.2020.100162
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Tracking HIV Rebound following Latency Reversal Using Barcoded HIV

Abstract: Summary HIV latency prevents cure of infection with antiretroviral therapy (ART) alone. One strategy for eliminating latently infected cells involves the induction of viral protein expression via latency-reversing agents (LRAs), allowing killing of host cells by viral cytopathic effects or immune effector mechanisms. Here, we combine a barcoded HIV approach and a humanized mouse model to study the effects of a designed, synthetic protein kinase C modulating LRA on HIV rebound. We show that administr… Show more

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Cited by 18 publications
(30 citation statements)
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“…In the current study we monitored viral loads for a much longer period of ~12 weeks after ART interruption, which likely explains why we found all mice receiving SUW133 alone eventually rebounded. Another difference is the use of TKO-BLT mice in the current study, which have lower levels of endogenous immune activation compared with the NSG-BLT used in the previous study 8,58 . This diminished basal immune activation may make induction of high-level HIV expression in latently infected cells by an LRA alone more difficult to achieve, necessitating the use of a specific "kill" agent to eliminate these cells as opposed to viral cytopathic effects alone.…”
Section: Discussionmentioning
confidence: 92%
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“…In the current study we monitored viral loads for a much longer period of ~12 weeks after ART interruption, which likely explains why we found all mice receiving SUW133 alone eventually rebounded. Another difference is the use of TKO-BLT mice in the current study, which have lower levels of endogenous immune activation compared with the NSG-BLT used in the previous study 8,58 . This diminished basal immune activation may make induction of high-level HIV expression in latently infected cells by an LRA alone more difficult to achieve, necessitating the use of a specific "kill" agent to eliminate these cells as opposed to viral cytopathic effects alone.…”
Section: Discussionmentioning
confidence: 92%
“…NK cells also delay rebound of X4-tropic barcoded HIV. Next, we investigated whether HIV-1 barcoded technology could quantify the effect that allogeneic human peripheral blood NK cells had on rebounding viral clones after ART interruption 8,45 . As such, we recently developed a genetically barcoded HIV-1 containing a 21 bp genetic barcode inserted upstream of a hemagglutinin tag in the nonfunctional vpr region of the HIV strain NL-HA 8,46 , which is an X4-tropic near full-length, replication-competent, pathogenic strain of NL4-3 (Fig.…”
Section: Resultsmentioning
confidence: 99%
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“…Because identifying latent cells is challenging, many experimental latency systems include reporter genes and/or delete viral genes believed to be unnecessary for silencing and reactivation (33,34,52). For example, two prominent studies that used barcoded proviruses to track virus dissemination in animals used vpr-proviruses (33,52). The impact of this variation is not well understood.…”
Section: Discussionmentioning
confidence: 99%
“…This suggests that the observed effect of vpr in our in vitro system may also contribute to shaping the persistent latent reservoir in patients. If so, existing animal studies that have studied latency and reactivation using vpr-proviruses may largely be tracking the properties of proviruses that are eliminated during natural infection (52).…”
Section: Discussionmentioning
confidence: 99%