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Fv1 restriction and retrovirus vaccine immunity in Apobec3-deficient 129P2 mice.

Kalani Halemano, Bradley S Barrett, Sam X Li, Michael S Harper, Diana S Smith, Karl J Heilman, Mario L Santiago

PloS one 2013


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  • Apobec3 (7)
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  • mice balb c (1)
  • mice knockout (1)
  • retrovirus (11)
  • Rfv3 (4)
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    Understanding the host genetics of the immune response in retrovirus infection models could provide insights for basic HIV vaccine discovery. In Friend retrovirus (FV) infection of mice, Fv1 differentially inhibits N-tropic versus B-tropic FV infection by mediating a capsid-dependent post-entry block, Fv2 susceptibility governs splenomegaly induction, and Rfv3 resistance primes a stronger neutralizing antibody response due to more potent Apobec3 activity. Apobec3 polymorphisms in inbred mouse strains correlate with Rfv3 resistance and susceptibility, with one unresolved exception. The 129/OlaHsd (129P2) mouse strain is Fv2 and Rfv3 susceptible based on genotyping, but infection of 129P2 mice with B-tropic FV resulted in strong neutralizing antibody responses and no splenomegaly. Here we confirm that 129P2 mice are Fv1(nr/nr), explaining its resistance to B-tropic FV. Infection of 129P2 mice with NB-tropic FV, which can efficiently infect mice independent of Fv1 genotype, resulted in severe splenomegaly, high levels of viremia and weak neutralizing antibody responses regardless of Apobec3 status. Notably, high-dose B-tropic FV infection of 129P2 Apobec3-deficient mice induced significant adaptive immune responses and conferred high levels of protection following challenge with pathogenic NB-tropic FV. This immunological protection complemented previous studies that N-tropic FV can act as a live-attenuated vaccine in Fv1 (b/b) mice. Altogether, the results obtained in 129P2 mice strengthen the conclusion that Rfv3 is encoded by Apobec3, and highlight Fv1 incompatibility as a retroviral vaccine paradigm in mice. Due to its susceptibility to disease that allows for pathogenic challenge studies, B-tropic FV infection of 129P2 mice may be a useful model to study the immunological pathways induced by retroviral capsid restriction.

    Citation

    Kalani Halemano, Bradley S Barrett, Sam X Li, Michael S Harper, Diana S Smith, Karl J Heilman, Mario L Santiago. Fv1 restriction and retrovirus vaccine immunity in Apobec3-deficient 129P2 mice. PloS one. 2013;8(3):e60500

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    PMID: 23533681

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