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Antibody prophylaxis may mask subclinical SIV infections in macaques

Author

Listed:
  • Christopher A. Gonelli

    (National Institutes of Health)

  • Hannah A. D. King

    (National Institutes of Health
    Walter Reed Army Institute of Research
    Henry M. Jackson Foundation for the Advancement of Military Medicine)

  • SungYoul Ko

    (National Institutes of Health)

  • Christine M. Fennessey

    (Frederick National Laboratory for Cancer Research)

  • Nami Iwamoto

    (National Institutes of Health)

  • Rosemarie D. Mason

    (National Institutes of Health)

  • Ashley Heimann

    (National Institutes of Health)

  • Dillon R. Flebbe

    (National Institutes of Health)

  • John-Paul Todd

    (National Institutes of Health)

  • Kathryn E. Foulds

    (National Institutes of Health)

  • Brandon F. Keele

    (Frederick National Laboratory for Cancer Research)

  • Jeffrey D. Lifson

    (Frederick National Laboratory for Cancer Research)

  • Richard A. Koup

    (National Institutes of Health)

  • Mario Roederer

    (National Institutes of Health)

Abstract

Broadly neutralizing antibodies (bNAbs) show potential to prevent human immunodeficiency virus (HIV-1) infection in humans1. However, there are limited data on the antibody concentrations required to prevent infection. Clinical trials of bNAb prophylaxis have demonstrated partial efficacy2, but the sampling frequency typically does not allow precise timing of infection events and concurrent antibody levels. Here, using simian immunodeficiency virus (SIV) infection of rhesus macaques, we show that although potent bNAbs can delay the onset of acute viremia, subclinical infections occur while bNAb levels remain high. Serial SIV challenge of monkeys given partially and fully neutralizing bNAbs revealed that ‘viral blips’—low and transient plasma viremia—often occur while serum bNAb concentrations are well above currently accepted protective levels. To understand the precise timing of the infections resulting in such blips, we performed plasma viral sequencing on monkeys that were serially challenged with genetically barcoded SIV after bNAb administration. These analyses showed that subclinical infections occurred in most animals that were given potent bNAb prophylaxis. These subclinical infections occurred while antibody concentrations were 2- to 400-fold higher than the levels required to prevent fully viremic breakthrough infection. This study demonstrates that immunoprophylaxis can mask subclinical infections, which may affect the interpretation of prophylactic HIV-1 bNAb clinical trials.

Suggested Citation

  • Christopher A. Gonelli & Hannah A. D. King & SungYoul Ko & Christine M. Fennessey & Nami Iwamoto & Rosemarie D. Mason & Ashley Heimann & Dillon R. Flebbe & John-Paul Todd & Kathryn E. Foulds & Brandon, 2025. "Antibody prophylaxis may mask subclinical SIV infections in macaques," Nature, Nature, vol. 639(8053), pages 205-213, March.
  • Handle: RePEc:nat:nature:v:639:y:2025:i:8053:d:10.1038_s41586-024-08500-y
    DOI: 10.1038/s41586-024-08500-y
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