Immune modulator N-803 does not control HIV rebound, suggesting a combination approach is needed for a functional cure

Most people with HIV who received the immune-modulating drug N-803 (Anktiva), with or without broadly neutralising antibodies (bnAbs), did not experience delayed viral rebound after stopping antiretroviral treatment, but they did show some favourable changes in immune response and the viral reservoir, according to a set of posters presented at the Conference on Retroviruses and Opportunistic Infections (CROI 2026) in Denver.

These results – which conflict with findings reported at a conference last year – add to the growing evidence that a combination approach will be needed for a functional cure, or long-term remission without antiretrovirals.

Antiretroviral therapy (ART) can keep HIV suppressed indefinitely, but the virus inserts its genetic blueprints – known as a provirus – into CD4 T-cells and establishes a long-lasting viral reservoir that is nearly impossible to eradicate. Cure researchers have tried many different strategies to control the virus, shrink the reservoir and boost immune response, but so far progress has been modest.

N-803, from ImmunityBio, is an interleukin 15 (IL-15) receptor ‘superagonist’ that activates natural killer (NK) cells and CD8 killer T-cells and enhances CD4 helper T-cell activity and proliferation of memory T-cells. The US Food and Drug Administration approved N-803 as a treatment for bladder cancer in 2024, and Saudi Arabia approved it last month for advanced lung cancer. It is currently being studied for several other malignancies, often in combination with immune checkpoint inhibitors, in an effort to strengthen immune responses against tumours. Early research suggests N-803 may also help the immune system fight HIV and might reactivate latent virus in the reservoir.

Three clinical trials – ACTG A5386 (NCT04340596), a study sponsored by Rockefeller University (NCT05245292) and the Thai RV550 study – assessed whether N-803, with or without bnAbs, could delay viral rebound after antiretroviral treatment interruption and boost immune response against HIV. Therapeutic bnAbs are manufactured versions of specialised antibodies that target conserved parts of the virus.

At last summer’s International AIDS Society Conference on HIV Science (IAS 2025), researchers presented initial findings from the Rockefeller trial, which tested N-803 plus two bnAbs, 3BNC117-LS and 10-1074-LS. That study enrolled 28 people with chronic HIV infection on stable ART with a sustained undetectable viral load. They received a single IV infusion of the bnAbs followed by up to eight injections of N-803 three weeks apart. Two days after bnAb administration, they started a closely monitored analytical treatment interruption (ATI).

Four people resumed their antiretrovirals before viral rebound occurred, and ten experienced early viral rebound as expected after stopping treatment. But of these ten and another 14 people who also did not restart treatment prior to rebound, 58% remained off ART at 24 weeks, 29% were still off at 48 weeks and three (13%) did not need to resume ART even at 72 weeks, including one who remained off antiretrovirals for 125 weeks at the time of the report.

ACTG A5386

At CROI, however, researchers with the other two trials did not report such encouraging results.

Dr R. Brad Jones from Weill Cornell Medicine in New York and colleagues presented findings from ACTG A5386, sponsored by the US National Institutes of Allergy and Infectious Diseases. This study included 48 adults with chronic HIV infection who were on ART with viral suppression for more than 96 weeks. Most (90%) were men and the median age was 50 years. They were tested for sensitivity to two bnAbs, VRC07-523-LS and 10-1074-LS. The 23 participants whose HIV was sensitive to one or both bnAbs received them along with N-803, while 25 people who were not sensitive received only N-803.

The bnAbs were administered at the start of the study, followed by up to eight doses of N-803 given three weeks apart. Both therapies were generally safe and well tolerated, but eight people developed severe neutropenia (white blood cell deficiency) thought to be possibly attributable to N-803.

In contrast to the Rockefeller study, which started an ATI two days after bnAb administration, ACTG A5386 participants stayed on their antiretrovirals while receiving the bnAbs and N-803. At 52 weeks, 19 people who got both the bnAbs and N-803 started a treatment interruption. (This poster did not report ATI results for those who got only N-803.)

Of these 19, seven requested to restart their antiretrovirals and six experienced viral rebound (above 1000 copies). Only one person (5%) met the primary endpoint of a viral load below 200 at eight weeks off ART, and three had a viral load below 1000 at that timepoint. One participant restarted antiretrovirals at 24 weeks and one remains off treatment.

“N-803 plus bnAbs did not lead to viral control after ART cessation as hypothesised,” the researchers concluded. They are further investigating what factors might be associated with viral control in the two people with longer remission.

However, N-803 did appear to have some effect on the viral reservoir and immune responses against HIV. In an analysis of 42 people performed after five doses of N-803, 70% showed a transient decline in intact provirus HIV DNA (median -0.19 log with N-803 alone; -0.25 log with N-803 plus bnAbs). Intact reservoir levels rebounded to near baseline by ten weeks after completion of dosing.

In a second analysis, Itzayana Miller, also from Weill Cornell, and colleagues looked at T-cell features associated with viral control in ACTG A5386. According to this poster, two people who received only N-803 maintained a viral load below 1000 for 24 weeks, in addition to those described by Jones who got both N-803 and bnAbs.

Those who received N-803 with or without bnAbs showed modest shifts toward ‘stem-like’ T-cells (TCF-1+ and stem cell memory CD8 cells) with a high capacity for proliferation, more potent activity against HIV and less evidence of exhaustion. This type of T-cell has been previously linked to post-treatment control of HIV. What’s more, those with evidence of HIV control showed high proliferation of Gag- and Nef-specific CD8 T cells and Gag- and Pol-specific CD4 T cells.

RV550

The phase II RV550 trial, sponsored by the US Military HIV Research Program and conducted by the Thai Red Cross, took a different approach, evaluating the effect of N-803, in combination with antiretrovirals, on the viral reservoir in people with acute HIV infection. People who start treatment very soon after acquiring HIV have a smaller reservoir and a better chance of achieving remission.

In step 1 of this study, 12 participants were randomly assigned to receive antiretrovirals alone or ART plus three doses of N-803 administered three weeks apart. In step 2, seven of them received a dose of N-803 regardless of randomisation and started an ATI.

The researchers previously reported that people who received ART plus N-803 experienced faster viral load decline than those on ART alone, but there was no difference in HIV DNA in the blood. The study presented at CROI showed that with additional analysis of lymph nodes and other tissues, the N-803 group did show a substantial decrease in viral RNA. However, there were no significant differences between the two groups in time to viral rebound, peak viral load, time to ART re-initiation or how long it took to re-suppress the virus after resuming antiretrovirals.

“N-803 was safe but did not significantly alter viral rebound kinetics during ATI,” the researchers concluded. “However, N-803 decreased viral RNA in lymph nodes by 50-fold and may be effective in future combinatorial strategies.”

Taken together, these findings offer further evidence that combination approaches have the best prospects for producing long-term HIV remission that could allow people to stay off antiretrovirals for several months or longer.

N-803 might be a component of such functional cure strategies, but bispecific antibody-like constructs that deliver IL-15 directly to memory CD4 cells might hold even more promise. T4IL15 and T4IL15Δ, developed by Dr David Ho’s lab at the Aaron Diamond AIDS Research Center in New York, demonstrated “an unprecedented propensity to activate latent HIV-1,” according to the researchers.
 

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