Abstract Background Lenacapavir (LEN) is a novel long-acting injectable antiretroviral therapy (ART) drug for heavily treatment-experienced (HTE) people with HIV (PWH). However, real-world data on its use and outcomes are limited. We describe early real-world experience with LEN among HTE PWH across five clinics in Chicago, IL and Pittsburgh, PA. Methods We conducted a multi-center retrospective cohort study of HTE PWH who started LEN from November 13, 2020, through April 4, 2025. Demographic and clinical characteristics were collected, including previous ART regimens, HIV drug resistance mutations, HIV viral loads (VL), and self-reported adherence to optimized background regimen (OBR) after starting LEN. Results Forty-six individuals received at least one dose of LEN; most were cisgender men (61%), Black (72%), and had stable housing (87%) (Table 1). At initiation, their mean age was 52 years and on average had been living with HIV for 25 years. Extensive drug resistance was common: 34 had resistance to ≥2 NRTIs, 34 to ≥2 NNRTIs, 13 to ≥2 PIs, and 21 to ≥2 INSTIs; four showed resistance across all four drug classes. Among 23 individuals with viremia at LEN initiation (VL ≥200 c/mL), 91% achieved viral suppression during the observed period, with 70% doing so within the first 3 months (Figures 1 and 2). Two individuals remained unsuppressed after LEN due to self-reported OBR non-adherence. All individuals without viremia at initiation maintained viral suppression throughout follow-up. Before LEN, 30% had a genotypic susceptibility score indicating their regimen had fewer than two fully active agents; after initiation, all had regimens with at least two active agents (Table 2). Nearly all individuals (91%) remained on LEN through the observation period; median time on LEN was 373 days (IQR 123–576). Discontinuations (n=4) were due to OBR non-adherence, injection site reaction, hospice entry, or loss to follow-up. Conclusion In this real-world cohort, LEN-based regimens resulted in high rates of virologic suppression among HTE PWH. Our findings support LEN as a promising salvage therapy when paired with an active OBR. As LEN use expands, targeted implementation strategies will be critical to address adherence challenges, manage side effects, and optimize sustained treatment success for HTE populations. Disclosures Aniruddha Hazra, MD, Abbott Laboratories: Advisor/Consultant|Gilead Sciences, Inc: Advisor/Consultant|Gilead Sciences, Inc: Grant/Research Support|GSK/ViiV Healthcare: Advisor/Consultant
Kaperak et al. (Thu,) studied this question.