Nature Communications (May 2025)
Autologous HIV-specific T cell therapy targeting conserved epitopes is well-tolerated in six adults with HIV: an open-label, single-arm phase 1 study
- Danielle K. Sohai,
- Michael D. Keller,
- Patrick J. Hanley,
- Fahmida Hoq,
- Divyesh Kukadiya,
- Anushree Datar,
- Emily Reynolds,
- Dennis C. Copertino,
- Christopher Lazarski,
- Chase D. McCann,
- Jay Tanna,
- Abeer Shibli,
- Haili Lang,
- Anqing Zhang,
- Pamela A. Chansky,
- Cecilia Motta,
- Tan T. Huynh,
- Bridget Dwyer,
- Andrew Wilson,
- Rebecca Lynch,
- Talia M. Mota,
- Winiffer D. Conce Alberto,
- Zabrina L. Brumme,
- Natalie N. Kinloch,
- Conrad Russell Y. Cruz,
- Lynsay MacLaren Ehui,
- Sarah Henn,
- R. Brad Jones,
- Catherine M. Bollard
Affiliations
- Danielle K. Sohai
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Michael D. Keller
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Patrick J. Hanley
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Fahmida Hoq
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Divyesh Kukadiya
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Anushree Datar
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Emily Reynolds
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Dennis C. Copertino
- Infectious Diseases Division, Department of Medicine, Weill-Cornell Medicine
- Christopher Lazarski
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Chase D. McCann
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Jay Tanna
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Abeer Shibli
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Haili Lang
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Anqing Zhang
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Pamela A. Chansky
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Cecilia Motta
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Tan T. Huynh
- Infectious Diseases Division, Department of Medicine, Weill-Cornell Medicine
- Bridget Dwyer
- Integrated Biomedical Sciences, Department of Microbiology, Immunology, and Tropical Medicine, and Department of Pediatrics, The George Washington University
- Andrew Wilson
- Integrated Biomedical Sciences, Department of Microbiology, Immunology, and Tropical Medicine, and Department of Pediatrics, The George Washington University
- Rebecca Lynch
- Integrated Biomedical Sciences, Department of Microbiology, Immunology, and Tropical Medicine, and Department of Pediatrics, The George Washington University
- Talia M. Mota
- Infectious Diseases Division, Department of Medicine, Weill-Cornell Medicine
- Winiffer D. Conce Alberto
- Infectious Diseases Division, Department of Medicine, Weill-Cornell Medicine
- Zabrina L. Brumme
- Faculty of Health Sciences, Simon Fraser University
- Natalie N. Kinloch
- Faculty of Health Sciences, Simon Fraser University
- Conrad Russell Y. Cruz
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- Lynsay MacLaren Ehui
- Whitman-Walker Health
- Sarah Henn
- Whitman-Walker Health
- R. Brad Jones
- Infectious Diseases Division, Department of Medicine, Weill-Cornell Medicine
- Catherine M. Bollard
- Center for Cancer and Immunology Research, and Division of Biostatistics and Study Methodology, Children’s National Hospital
- DOI
- https://doi.org/10.1038/s41467-025-59810-2
- Journal volume & issue
-
Vol. 16,
no. 1
pp. 1 – 15
Abstract
Abstract Novel cellular therapies may enable HIV control or cure. HIV-specific T cells targeting conserved immunogenic protein regions of HIV Gag/Pol and the entirety of HIV Nef, termed HST-NEETs, eliminate HIV infected cells in vitro. Here we enroll seven participants in an open-label, single-arm phase 1 study (NCT03485963) to evaluate the safety (primary endpoint) of two autologous administrations of HST-NEET products without prescribed lymphodepletion. Adults with well-controlled HIV on anti-retroviral therapy are eligible. Six participants completed safety monitoring. No serious product-related toxicities are observed. Secondary endpoints are to assess expansion and persistence of HIV-reactive T cell clones, and changes to the HIV reservoir for each infused participant. HIV-specific T cell and HIV anti-Env antibody responses increase in two participants after infusion two. A trend towards decreasing levels of intact proviruses is observed in 2 participants. Three participants show persistence of HIV-reactive, product-associated T cell clones for ≥40 weeks post infusions. HST-NEETs infusions are well-tolerated. Future trials are needed to evaluate the efficacy of HST-NEETs in this population.
