Mary Jo Florey scite author profile

In an earlier study we found that pigtailed macaques (Macaca nemestrina) that were experimentally infected with human immunodeficiency virus type 1 (HIV-1) initially became viremic and seroconverted, but HIV-1 replication diminished markedly over time. In an attempt to develop a longer term pathogenic model, blood from HIV-1-infected macaques was serially transfused into three groups of naive macaques. Transfer was successful through two transfusions as shown by repeated virus isolations and confirmed by the development of cell-free plasma viremia and by seroconversion. Three to five weeks after transfusion, plasma levels of HIV-1 RNA from several macaques in the first two groups exceeded those of the initially inoculated macaques. However, animals in the third group had diminished RNA levels, were virus culture negative, and did not seroconvert. Sequence analyses of env-region clones from infected animals revealed only minimal changes over the course of the passages. These results confirm HIV-1 replication in M. nemestrina during the acute phase of infection. However, adaptation of HIV-1 to a macaque-pathogenic variant did not occur during serial passage, possibly because the animals were able to restrict HIV-1 replication below a level required for a pathogenic variant to emerge. Whether such containment is a function of the host's immune response or a virus cell incompatibility remains to be determined.

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Enhanced replication of HIV‐1 in vivo in pigtailed macaques (Macaca nemestrina)

Bosch

Schmidt

Chen

et al. 2000

J of Medical Primatology

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Non-human primate models for acquired immunodeficiency syndrome (AIDS) are important for studies of prevention and intervention strategies. Ideally, such models would make use of human immunodeficiency virus type 1 (HIV-1) and animals that are readily available for research. HIV-1 was obtained from an infected macaque, and passaged sequentially in three groups of two Macaca nemestrina neonates each. Evidence for enhanced viral replication was first found in one of the group 2 animals, and in both group 3 animals. Observations that underlie this conclusion are sustained viral recovery from peripheral blood mononuclear cells (PBMCs), increased and accelerated production of antiviral antibodies, and the ability to detect plasma viral ribonucleic acid (RNA) months after infection. There was no evidence of CD4 depletion in any of the animals during the follow-up period. These data suggest that a useful non-human primate model for AIDS can be attained in pigtailed macaques (M. nemestrina).

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Effect of BCG on Friend Disease Virus in Mice

et al. 1971

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Modified E-rosette test for detection of total and active rosette-forming lymphocytes

Florey¹,

Peetoom²

1976

Journal of Immunological Methods

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Mary Jo Florey

Acute Infection of Macaca nemestrina by Human Immunodeficiency Virus Type 1

Serialin VivoPassage of HIV-1 Infection inMacaca nemestrina

Enhanced replication of HIV‐1 in vivo in pigtailed macaques (Macaca nemestrina)

Effect of BCG on Friend Disease Virus in Mice

Modified E-rosette test for detection of total and active rosette-forming lymphocytes

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