2013
DOI: 10.1371/journal.pone.0054871
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Selective Expansion of Viral Variants following Experimental Transmission of a Reconstituted Feline Immunodeficiency Virus Quasispecies

Abstract: Following long-term infection with virus derived from the pathogenic GL8 molecular clone of feline immunodeficiency virus (FIV), a range of viral variants emerged with distinct modes of interaction with the viral receptors CD134 and CXCR4, and sensitivities to neutralizing antibodies. In order to assess whether this viral diversity would be maintained following subsequent transmission, a synthetic quasispecies was reconstituted comprising molecular clones bearing envs from six viral variants and its replicativ… Show more

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Cited by 9 publications
(11 citation statements)
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“…The selective pressure for the emergence of CRD2-independent viruses may be escape from humoral or cellular immunity, with the accrued mutations in Env impacting on the virus-receptor interaction [ 30 , 32 ]. Consistent with this hypothesis, when cats were challenged with a reconstituted viral quasispecies containing equal titres of clonal variants with either CRD2-dependent or CRD2-independent Envs (early and late phenotypes), the CRD2-dependent viruses expanded preferentially in vivo while the CRD2-independent viruses failed to thrive [ 33 ].…”
Section: Resultsmentioning
confidence: 98%
“…The selective pressure for the emergence of CRD2-independent viruses may be escape from humoral or cellular immunity, with the accrued mutations in Env impacting on the virus-receptor interaction [ 30 , 32 ]. Consistent with this hypothesis, when cats were challenged with a reconstituted viral quasispecies containing equal titres of clonal variants with either CRD2-dependent or CRD2-independent Envs (early and late phenotypes), the CRD2-dependent viruses expanded preferentially in vivo while the CRD2-independent viruses failed to thrive [ 33 ].…”
Section: Resultsmentioning
confidence: 98%
“…These CRD2-independent isolates, which are characteristic of the later stages of FIV infection, were also shown to be less efficient for transmission and replication during acute infection when compared to CRD2-dependent isolates in experimental infection studies. These findings generated a hypothesis that CRD2-dependent FIV isolates, which are efficiently transmitted in vivo and able to achieve higher virus loads during early infection, may be analogous to CCR5-dependent HIV-1 isolates that also transmit much more efficiently during primary HIV-1 infection of humans when compared to later-emerging CXCR4-tropic variants in HIV-1 infection [49,50]. Specific CD4+ T cell subsets that may be specific targets for these CRD2-dependent FIV isolates and their role in viral pathogenesis remain to be determined.…”
Section: Fiv Receptor Usagementioning
confidence: 99%
“…This hypothesis was supported by the findings from a study conducted in cats experimentally inoculated with reconstituted quasispecies composed of GL8 and variants containing CRD2-dependent or CRD2-independent Envs [ 44 ]. Throughout the 21-week period of study, the variants of GL8 containing CRD2-dependent Envs replicated faster and selectively expanded in all cats.…”
Section: Crd2-independent Variants Are a Consequence Not The Causmentioning
confidence: 65%
“…Throughout the 21-week period of study, the variants of GL8 containing CRD2-dependent Envs replicated faster and selectively expanded in all cats. It was demonstrated that the failure to replicate by the CRD2-independent variants was not associated with either the presence of neutralising antibodies or cell-mediated immune responses [ 44 ], suggesting that the switch in receptor phenotype also led to decreased replicative fitness.…”
Section: Crd2-independent Variants Are a Consequence Not The Causmentioning
confidence: 99%