Viruses (Jun 2024)

Production and Immunogenicity of FeLV Gag-Based VLPs Exposing a Stabilized FeLV Envelope Glycoprotein

  • Raquel Ortiz,
  • Ana Barajas,
  • Anna Pons-Grífols,
  • Benjamin Trinité,
  • Ferran Tarrés-Freixas,
  • Carla Rovirosa,
  • Víctor Urrea,
  • Antonio Barreiro,
  • Anna Gonzalez-Tendero,
  • Maria Rovira-Rigau,
  • Maria Cardona,
  • Laura Ferrer,
  • Bonaventura Clotet,
  • Jorge Carrillo,
  • Carmen Aguilar-Gurrieri,
  • Julià Blanco

DOI
https://doi.org/10.3390/v16060987
Journal volume & issue
Vol. 16, no. 6
p. 987

Abstract

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The envelope glycoprotein (Env) of retroviruses, such as the Feline leukemia virus (FeLV), is the main target of neutralizing humoral response, and therefore, a promising vaccine candidate, despite its reported poor immunogenicity. The incorporation of mutations that stabilize analogous proteins from other viruses in their prefusion conformation (e.g., HIV Env, SARS-CoV-2 S, or RSV F glycoproteins) has improved their capability to induce neutralizing protective immune responses. Therefore, we have stabilized the FeLV Env protein following a strategy based on the incorporation of a disulfide bond and an Ile/Pro mutation (SOSIP) previously used to generate soluble HIV Env trimers. We have characterized this SOSIP-FeLV Env in its soluble form and as a transmembrane protein present at high density on the surface of FeLV Gag-based VLPs. Furthermore, we have tested its immunogenicity in DNA-immunization assays in C57BL/6 mice. Low anti-FeLV Env responses were detected in SOSIP-FeLV soluble protein-immunized animals; however, unexpectedly no responses were detected in the animals immunized with SOSIP-FeLV Gag-based VLPs. In contrast, high humoral response against FeLV Gag was observed in the animals immunized with control Gag VLPs lacking SOSIP-FeLV Env, while this response was significantly impaired when the VLPs incorporated SOSIP-FeLV Env. Our data suggest that FeLV Env can be stabilized as a soluble protein and can be expressed in high-density VLPs. However, when formulated as a DNA vaccine, SOSIP-FeLV Env remains poorly immunogenic, a limitation that must be overcome to develop an effective FeLV vaccine.

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