How NPRC Research Accelerated HIV Advances From 2020–2025

From breakthroughs in prevention to promising treatments, the National Primate Research Centers (NPRCs) have played a crucial role in advancing HIV research. Working with nonhuman primates, the closest biomedical model to humans, NPRC researchers have tackled some of HIV’s biggest challenges: viral persistence, brain invasion, co-infections and the limits of current therapies. Together, these discoveries mark some of the most significant progress toward long-term remission and potential cures in decades.

Strengthening Vaccines and Early Prevention

NPRC advances include efforts to block infection before it starts. Researchers at the Emory National Primate Research Center (ENPRC) at Emory University showed that an Env-plus-Gag HIV vaccine regimen in rhesus macaques provided durable protection from SHIV, the simian version of HIV, even when neutralizing antibody levels were low. This finding expanded thinking around the types of immune responses a successful vaccine must generate.

At the same time, Oregon NPRC scientists found that leronlimab, a monoclonal antibody that blocks the CCR5 co-receptor, effectively prevented SHIV infection in nonhuman primate models. Already tested in human studies for viral suppression, the antibody also showed promise as a PrEP-style preventive option.

Targeting HIV’s Hidden Reservoirs

Because HIV hides in tissues the immune system can’t easily reach, several NPRC studies focused on uncovering and disrupting these viral reservoirs. ENPRC scientists discovered that the anti-inflammatory molecule IL-10 helps HIV-infected cells survive in lymph nodes. Blocking IL-10, alongside antiretroviral therapy (ART), reduced the number of infected reservoir cells, marking an important step toward weakening HIV’s stronghold.

Researchers at Emory NPRC also identified specialized follicle-infiltrating NK cells capable of entering B-cell follicles in lymph nodes, one of HIV’s most protected hiding places. These findings point toward future therapies that could guide immune cells directly into viral reservoir sites.

Additional “shock and kill” studies at Wisconsin NPRC showed that both latency-reversing drugs and checkpoint inhibitor combinations can reactivate dormant virus while nonhuman primates are on ART, laying groundwork for strategies that flush HIV out of hiding.

Immune-Based Therapies Move Toward Functional Cure

By 2024, several NPRC collaborations delivered results that brought the field closer to long-term remission without lifelong treatment. A landmark study testing N-803 (IL-15 superagonist) plus broadly neutralizing antibodies achieved long-lasting viral control in most SHIV-infected macaques even after ART was stopped. The findings have now progressed to early-phase human clinical trials.

Emory NPRC researchers also identified a particularly potent subset of CD8⁺ T cells (TCF1⁺CD39⁺) that excel at controlling SIV and resisting exhaustion. The importance of these cells has been confirmed also in people with HIV and may become powerful tools in future immunotherapies.

Understanding HIV in the Brain

Another major advancement came from California NPRC, where researchers discovered how HIV enters and persists in the brain. Their work showed that CD4 T cells can inadvertently carry virus into neural tissue, helping explain why HIV-associated neurocognitive disorders persist even when ART is effective.

Addressing Co-Infections and Real-World Treatment Needs

HIV rarely exists in isolation. In 2025, Texas Biomed and the Southwest NPRC demonstrated that a promising tuberculosis therapy did not interfere with combined antiretroviral therapy (cART) used to treat HIV, supporting its safe use in people co-infected with HIV and TB. Because the drug is already FDA-approved for use in cancer patients, it could accelerate potential approval for TB/HIV treatment compared to developing an entirely new drug.

A Path Toward Remission

Building on these advances, Emory NPRC researchers reported one of the strongest signals yet that a functional cure for HIV may be achievable. In a stringent SIV model, a targeted combination therapy, blocking two negative regulators of the immune system, IL-10 and PD-1, enabled durable control of viral rebound in 9 of 10 nonhuman primates for six months after ART ended, an unprecedented result that strengthens the path toward future human trials. This is a direct proof of concept that the immune system can be harnessed with immune-based interventions to control HIV.

The Bottom Line

Between 2020 and 2025, NPRC research meaningfully advanced the HIV landscape. Through innovative vaccine approaches, better understanding of persistence, targeted immune strategies and real-world treatment insights, the NPRCs have laid essential groundwork for an era in which long-term HIV remission, and ultimately a cure, becomes an attainable goal.