1. Academic Validation
  2. Preclinical virology profiles of the HIV-1 capsid inhibitors VH4004280 and VH4011499

Preclinical virology profiles of the HIV-1 capsid inhibitors VH4004280 and VH4011499

  • Antimicrob Agents Chemother. 2025 Oct;69(10):e0030925. doi: 10.1128/aac.00309-25.
Chunfu Wang 1 Haichang Huang 1 Lourdes Valera 1 Kyle Parcella 2 Christiana Iwuagwu 2 Brian McAuliffe 1 Paul J Falk 1 Donald R O'Boyle Ii 1 Ronald E Rose 1 Ricardo Ramírez Padilla 3 Chunxiang Wu 3 Yong Xiong 3 John Kadow 2 Umesh Hanumegowda 1 Luca Sardo 1 Eric P Gillis 2 Mark Krystal 1 Robert A Fridell 1
Affiliations

Affiliations

  • 1 Discovery Biology, ViiV Healthcare, Branford, Connecticut, USA.
  • 2 Discovery Chemistry, ViiV Healthcare, Branford, Connecticut, USA.
  • 3 Department of Molecular Biophysics and Biochemistry, Yale University, New Haven, Connecticut, USA.
Abstract

With its high degree of conservation and critical role in multiple steps of the HIV-1 life cycle, the HIV-1 capsid protein presents an attractive therapeutic target. Herein, the virologic properties of the HIV-1 capsid inhibitors VH4004280 (VH-280) and VH4011499 (VH-499), including potency, mechanisms of action, and resistance profiles, are described. VH-280 and VH-499 inhibited panels of HIV-1 laboratory strains and viruses containing capsid sequences from clinical isolates with half-maximal effective concentrations in the picomolar range. Time-of-addition experiments determined that the primary block to HIV-1 replication occurred after nuclear import and before integration; however, measurements of replication intermediates by quantitative polymerase chain reaction, Gag degradation, p24 release, and virion morphology by cryo-electron microscopy indicate that VH-280 and VH-499 also block nuclear import, total reverse transcript production, integration, virion assembly, and maturation. In vitro Resistance Selection identified Q67H, A105E, T107D/N, and combinations of these substitutions as conferring 6- to >5,000-fold reductions in susceptibility to both compounds. Certain resistance-associated mutations selected by Other capsid inhibitors also reduced susceptibility. Overall, the preclinical virology profiles and Other drug-like properties support the potential of VH-280 and VH-499 as long-acting agents for HIV-1 treatment and prevention.

Keywords

HIV-1; RAM; antiviral activity; capsid; mechanism of action; qPCR; resistance-associated mutation.

Figures
Products
  • Cat. No.
    Product Name
    Description
    Target
    Research Area
  • HY-159828
    99.97%, HIV-1 Inhibitor
    HIV