Abstract
Antiretroviral therapy (ART) for HIV-1 infection is life-long. Stopping therapy typically leads to the reignition of infection and progressive disease. In a major breakthrough, recent studies have shown that early initiation of ART can lead to sustained post-treatment control of viremia, raising hopes of long-term HIV-1 remission. ART, however, elicits post-treatment control in a small fraction of individuals treated. Strikingly, passive immunization with broadly neutralizing antibodies (bNAbs) of HIV-1 early in infection was found recently to elicit long-term control in a majority of SHIV-infected macaques, suggesting that HIV-1 remission may be more widely achievable. The mechanisms underlying the control elicited by bNAb therapy, however, remain unclear. Untreated infection typically leads to progressive disease. We hypothesized that viremic control represents an alternative but rarely realized outcome of the infection and that early bNAb therapy triggers a dynamical switch to this outcome. To test this hypothesis, we constructed a model of viral dynamics with bNAb therapy and applied it to analyse clinical data. The model fit quantitatively the complex longitudinal viral load data from macaques that achieved lasting control. The model predicted, consistently with our hypothesis, that the underlying system exhibited bistability, indicating two potential outcomes of infection. The first had high viremia, weak cytotoxic effector responses, and high effector exhaustion, marking progressive disease. The second had low viremia, strong effector responses, and low effector exhaustion, indicating lasting viremic control. Further, model predictions suggest that early bNAb therapy elicited lasting control via pleiotropic effects. bNAb therapy lowers viremia, which would also limit immune exhaustion. Simultaneously, it can improve effector stimulation via cross-presentation. Consequently, viremia may resurge post-therapy, but would encounter a primed effector population and eventually get controlled. ART suppresses viremia but does not enhance effector stimulation, explaining its limited ability to elicit post-treatment control relative to bNAb therapy.
Highlights
Current antiretroviral therapies (ART) for HIV-1 infection control viremia in infected individuals but are unable to eradicate the virus [1]
In a remarkable advance in HIV cure research, a recent study showed that 3 weekly doses of HIV-1 broadly neutralizing antibodies soon after infection kept viral levels controlled for years in most macaques treated
We predict that early broadly neutralizing antibodies (bNAbs) therapy suppresses viremia, which reduces exhaustion of cytotoxic effector cells, and enhances antigen uptake and effector stimulation
Summary
Current antiretroviral therapies (ART) for HIV-1 infection control viremia in infected individuals but are unable to eradicate the virus [1]. That functional cure can be achieved has been demonstrated by the VISCONTI trial, where a subset of patients, following early initiation of ART, maintained undetectable viremia long after the cessation of treatment [8]. Nishimura et al [10] found recently that early, short-term passive immunization with a combination of two HIV-1 broadly neutralizing antibodies (bNAbs) elicited lasting control of viremia in 10 of 13, or nearly 77%, of SHIV-infected macaques treated. This high success rate raises the prospect of achieving functional cure in all HIV-1 infected individuals using short-term bNAb therapy. Efforts have been initiated to develop immunotherapies that may further improve response rates in primate models [11,12,13,14] and to translate them to humans [15,16,17]
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
